Del Mar Photonics - Newsletter Fall 2010 - Newsletter Winter 2010
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Photonics West 2011: Presentations on photonics applications in mouse models research
Oxidative stress of photodynamic antimicrobial chemotherapy inhibits Candida 
albicans virulence 
Paper 7887-10 of Conference 7887
Date: Saturday, 22 January 2011
Time: 12:00 PM – 12:20 PM
Author(s): Ilka T. Kato, Renato A. Prates, Instituto de Pesquisas Energéticas e 
Nucleares (Brazil); George P. Tegos, The Univ. of New Mexico (United States) and 
Massachusetts General Hospital (United States) and Harvard Medical School 
(United States); Michael R. Hamblin, Massachusetts General Hospital (United 
States) and Harvard Medical School (United States) and Massachusetts Institute 
of Technology (United States); Martha Simões Ribeiro, Instituto de Pesquisas 
Energéticas e Nucleares (Brazil)
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In this study, the virulence of Candida albicans submitted to sublethal 
photodynamic inactivation was evaluated. C. albicans were exposed to sublethal 
photodynamic challenge using methylene blue as photosensitizer, associated with 
a diode laser irradiation (?=660nm). The parameters of irradiation were selected 
in causing no reduction of viable cells as sublethal photodynamic challenge. The 
potential effects of PACT on virulence determinants of C. albicans were 
investigated by analysis of germ tube formation and in vivo pathogenicity assays 
using a mice model for systemic infection. The oxidative damage promoted by 
sublethal photodynamic inactivation inhibited virulence factors and reduced in 
vivo pathogenicity of C. albicans.
Efficacy of continuous wave and pulsed wave transcranial laser therapy (TLT) in 
the treatment of Alzheimer's disease (AD) in an amyloid precursor protein 
transgenic mouse (APP Tg) model 
Paper 7887-19 of Conference 7887
Date: Saturday, 22 January 2011
Time: 5:00 PM – 5:20 PM
Author(s): Luis H. De Taboada, PhotoThera, Inc. (United States); Jin Yu, Salim 
El-Amouri, Medical Univ. of South Carolina (United States); Sebastiano 
Gattoni-Celli, Charleston VA Medical Ctr. (United States); Steven Richieri, 
Thomas McCarthy, PhotoThera, Inc. (United States); Jackson Streeter, Banyan 
Biomarkers, Inc. (United States); Mark S. Kindy, Medical Univ. of South Carolina 
(United States)
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Continuous Wave (CW) and Pulsed Wave (PW) TLT was tested for efficacy in a 
transgenic (Swedish/London) APP mouse model of AD. Administration of TLT was 
associated with a dose-dependent reduction in amyloid load and the numbers of Aß 
plaques. All TLT doses mitigated the behavioral deficits seen with advanced 
amyloid deposition and reduced the expression of inflammatory markers in the APP 
Tg mice. All TLT doses produced an increase in sAPP-a and a decrease in sAPP-ß 
levels consistent with inhibition of the ß-secretase activity. Oxygen 
consumption and ATP concentrations in the brains of APP Tg mice were 
significantly reduced compared to Wt mice, but essentially restored in the PW 
TLT treated APP mice. PW TLT induced a transient increase in c-fos protein 
expression, while Wt and APP Tg mice alone showed little to no c-fos activity. 
These studies suggest that TLT is a potential candidate for the treatment of AD.
Dual thermal ablation modality of solid tumors in a mouse model 
Paper 7901-34 of Conference 7901
Date: Monday, 24 January 2011
Time: 2:20 PM – 2:40 PM
Author(s): Gal Shafirstein, Eduardo G. Moros, K. Barnes, Leah Hennings, Jessica 
Weber, Beata Przybyla, Robert Griffin, Univ. of Arkansas for Medical Sciences 
(United States)
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The objective of this work is to develop a new combination therapy consisting of 
cryoablation and conductive high-temperature ablation(C/HTA), for enhanced 
thermal ablation of solid tumors. The C/HTA probe was tested, in Balb/c mice 
bearing solid 4T1 tumors, in comparison to cryoablation and high temperature 
ablation, only. The C/HTA device induced larger ablation zones, in comparison to 
either modality alone. The relatively high thermal conductivity of ice, in 
comparison to water and native tissue, and the reduction in the intracellular pH 
of the treated margins are assumed to be the main causes for the improved C/HTA 
outcomes. Grant support: Winthrop Rockefeller Cancer-Institute, Fashion- 
Footwear Association of New York.
Non-invasive multimodal confocal imaging of squamous cell carcinoma in mice 
Paper 7883A-18 of Conference 7883A
Date: Saturday, 22 January 2011
Time: 4:10 PM – 4:30 PM
Author(s): Anna N. Yaroslavsky, Univ. of Massachusetts Lowell (United States); 
Pawel A. Mroz M.D., Harvard Medical School (United States) and Massachusetts 
General Hospital (United States); Victor A. Neel, Massachusetts General Hospital 
(United States)
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We present reflectance and fluorescence confocal images acquired in vivo from 
squamous cell carcinomas (SCC) developed in SENCAR mice. 0.25 mg/ml aqueous MB 
was injected in anesthetized mice around cancerous areas. In vivo noninvasive 
imaging was performed using a multimodal confocal system. Reflectance images 
were acquired at 658 and 785 nm. Fluorescence images were excited at 658 nm and 
registered between 690 and 710 nm. Imaging results were compared to the 
respective H&E histopathology. Both reflectance and fluorescence images of SCC 
exhibited patterns close to those of human SCC and correlated well with 
histopathology.
Variations in the optical scattering properties of skin in murine animal models
Paper 7907-28 of Conference 7907
Date: Sunday, 23 January 2011
Time: 11:50 AM – 12:10 PM
Author(s): Katherine Calabro, Boston Univ. (United States); Allison Curtis, 
Jean-Rene Galarneau, Thomas Krucker, Novartis Institutes for Biomedical 
Research, Inc. (United States); Irving J. Bigio, Boston Univ. (United States)
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Direct and/or indirect measurement of mouse skin is common in the development of 
novel biomedical optics techniques. In this work we identify sources of 
experimental variation that may arise in these studies, indicating that care can 
be taken to avoid or compensate for their affects. Specifically, gender 
differences in skin thickness are found to cause differences in the reflectance 
and scattering coefficient value by up to a factor of two. Additionally, changes 
in the hair growth cycle are found to influence scattering strength due to 
changes in skin thickness, and also from melanin collection in hair follicles.
Study of photosensitizers pharmacokinetics in mouse tumor model by 
transillumination fluorescence imaging in vivo 
Paper 7886-30 of Conference 7886
Date: Sunday, 23 January 2011
Time: 4:10 PM – 4:30 PM
Author(s): Marina V. Shirmanova, Irina V. Balalaeva, Marina A. Sirotkina, N.I. 
Lobachevsky State Univ. of Nizhni Novgorod (Russian Federation); Anna G. Orlova, 
Ilya V. Turchin, Institute of Applied Physics (Russian Federation); Elena V. 
Zagaynova, Nizhny Novgorod State Medical Academy (Russian Federation)
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This work demonstrates the possibility of investigation of pharmacokinetics of 
photosensitizers by means of fluorescence transillumination imaging in vivo. The 
experiments were performed on transplantable mouse cervical carcinoma using 
three drugs: photosens, alasens and fotoditazin. Animals were scanned by a 
single source (semiconductor laser) and detector (FMP) pair in transilluminative 
configuration. Based on fluorescence imaging, we evaluated in vivo the main 
pharmacokinetics parameters: maximum tumor-uptake, half-life in tumor, 
clearance. The results on kinetics of photosensitizers in tumor obtained in vivo 
agreed with data of standard methods ex vivo.
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Comparison of fluorescence tomography of protease-activatable probes in mouse 
lung tumors with x-ray micro-CT 
Paper 7892-32 of Conference 7892
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Xiaofeng Zhang, Cristian Badea, A. Paiman Ghafoori, David Kirsch, Yi 
Qi, G. Allan Johnson, Duke Univ. (United States)
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Fluorescence tomography provides a noninvasive means to probe the biochemistry 
within living animals with high sensitivity and specificity. Detection of 
proteases signifies key diseases in cancer research. In this in vivo animal 
study, we adopted a protease-mediated activatable fluorescent imaging probe, 
ProSense 750. The 3D distributions of the fluorescent probe in the living 
animals was reconstructed using free-space fluorescence diffuse optical 
tomography, and subsequently compared to anatomical images obtained using x-ray 
micro-CT. It was observed that activation of the imaging probe was not 
completely accordant to tumor size.
Laser injury and in-vivo multimodal imaging using a mouse model 
Paper 7897-38 of Conference 7897
Date: Tuesday, 25 January 2011
Time: 4:00 PM – 4:20 PM
Author(s): Ginger M. Pocock, Air Force Research Lab. (United States); Adam 
Boretsky, Praveena Gupta, The Univ. of Texas Medical Branch (United States); 
Jeffrey W. Oliver, Air Force Research Lab. (United States); Massoud Motamedi, 
The Univ. of Texas Medical Branch (United States)
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A murine model was used to perform in vivo experiments of laser-induced thermal 
damage to the retina. The expression kinetics and protein localization of 
biomarkers after laser induced injury to the retina and skin would provide a 
better understanding of the laser exposure levels at which the tissue becomes 
"stressed" and may be useful to detect sub-threshold laser damage that may or 
may not manifest as a visible lesion. A Heidelberg Spectralis HRA with a 
spectral domain optical coherence tomographer (OCT) was used to obtain images of 
the fundus and obtain cross-sectional views of the retina. Subthreshold and 
threshold lesions were observed using the OCT, infrared (IR) reflectance, and 
autofluorescence imaging modalities to observe lesion appearance. Volumetric 
representations of the retina were created to visualize lesion localization of 
damage.
Development and validation of a combined photoacoustic micro-ultrasound system 
for in-vivo oxygen saturation estimation 
Paper 7899-84 of Conference 7899
Date: Tuesday, 25 January 2011
Time: 5:30 PM – 5:45 PM
Author(s): Andrew Needles, Andrew Heinmiller, Pinhas Ephrat, David Bates, Corina 
Bilan-Tracey, Catherine Theodoropoulos, Desmond Hirson, Visualsonics Inc. 
(Canada); F. Stuart Foster, Sunnybrook Health Sciences Ctr. (Canada)
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Photoacoustic (PA) imaging can estimate the spatial distribution of oxygen 
saturation (SO2) in blood, and be co-registered with B-Mode images of the 
surrounding anatomy. This talk will focus on the development of a PA imaging 
mode on a commercially available array based micro-ultrasound (µUS) system that 
is capable of creating such images. Beamforming techniques, mode-interleaving, 
digital sampling and signal processing will be described, along with a new 
technique for in vivo validation of PA-SO2 estimation.
Imaging of hyaloid vessels in mouse embryonic eye with swept source optical 
coherence tomography 
Paper 7885-6 of Conference 7885
Date: Saturday, 22 January 2011
Time: 9:30 AM – 9:45 AM
Author(s): Kirill V. Larin, Univ. of Houston (United States)
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Throughout much of embryonic development, the mammalian lens is surrounded by a 
hyaloid vascular system. This vasculature is considered vital for the maturation 
and growth of the lens. OCT is a 3D imaging modality, which has the capability 
of producing high resolution (~8µm) images with an imaging depth of up to 3 mm. 
We tested the capability of OCT to perform live 3D imaging of the hyaloid 
vasculature in the embryonic eye in utero. Our results suggest that OCT can be 
used to understand the development and progression of hyaloid vasculature in the 
vitreous region of the eye.
Cortical blood flow imaging of mouse stroke model by high-speed spectral OCT 
Paper 7883E-109 of Conference 7883E
Date: Saturday, 22 January 2011
Time: 4:00 PM – 4:20 PM
Author(s): Ireneusz Grulkowski, Nicolaus Copernicus Univ. (Poland); Grzegorz 
Wilczynski, Nencki Institute of Experimental Biology (Poland); Danuta Bukowska, 
Maciej Szkulmowski, Nicolaus Copernicus Univ. (Poland); Jakub Wlodarczyk, Nencki 
Institute of Experimental Biology (Poland); Karol Karnowski, Daniel Ruminski, 
Andrzej A. Kowalczyk, Maciej Wojtkowski, Nicolaus Copernicus Univ. (Poland)
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We have developed and applied a high-speed spectral OCT system to image small 
animal brains. OCT imaging with high temporal and spatial resolution enabled 
cortical blood flow visualization. We imaged the brain vascular network of an 
anesthetized mouse stroke model. We demonstrated the impact of induced stroke on 
the brain vasculature. The preliminary studies have revealed local ischemia in 
the areas of the stroke.
In-utero imaging of mouse embryonic development with optical coherence 
tomography 
Paper 7889-9 of Conference 7889
Date: Monday, 24 January 2011
Time: 11:00 AM – 11:15 AM
Author(s): Saba H. Syed, Univ. of Houston (United States); Irina V. Larina, Mary 
E. Dickinson, Baylor College of Medicine (United States); Kirill V. Larin, Univ. 
of Houston (United States)
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Embryonic imaging is the most important tool in understanding and investigating 
developmental diseases. Mouse embryos have long served as an ideal model for the 
study of mammalian embryonic developmental processes. OCT is a promising 
technique introduced recently to developmental biology. In this study we 
introduce OCT as a novel technique to image live mouse embryos from stage 12.5 
through 17.5 days post-coitus (dpc). This study suggest that OCT can serve as a 
powerful tool to image mouse embryos with a resolution of ~8 µm and can help in 
understanding abnormalities in developmental processes caused by mutations, or 
toxic drugs.
Visualization of mouse kidney perfusion with multispectral optoacoustic 
tomography (MSOT) at video rate 
Paper 7899-39 of Conference 7899
Date: Monday, 24 January 2011
Time: 11:15 AM – 11:30 AM
Author(s): Andreas Buehler, Eva Herzog, Daniel Razansky, Vasilis Ntziachristos, 
Helmholtz Zentrum München GmbH (Germany)
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We report herein on a novel multi-spectral optoacoustic tomography (MSOT) system 
for deep tissue small animal imaging. The previously undocumented capacity of 
whole body optoacoustic tomography at video rate has been demonstrated by 
visualizing mouse kidney perfusion using Indocyanine Green in vivo.
Imaging necrosis in mouse models of muscular dystrophy with three-dimensional 
optical coherence tomography 
Paper 7889-12 of Conference 7889
Date: Monday, 24 January 2011
Time: 11:45 AM – 12:00 PM
Author(s): Blake R. Klyen, Thea Shavlakadze, Miranda D. Grounds, David D. 
Sampson, The Univ. of Western Australia (Australia)
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We report the use of three-dimensional optical coherence tomography (3D-OCT) in 
conjunction with Evans blue dye, a marker for muscle fiber permeability, used to 
guide the 3D-OCT imaging. We apply this to imaging mouse skeletal muscle tissue 
from exercise-induced damage models of dystropathology in human muscular 
dystrophy. Images are presented that show the ability of 3D-OCT to identify 
lesions, regions of necrosis and inflammation, within large volumes of skeletal 
muscle tissue, and differentiate these from the surrounding intact muscle 
fibers. These results demonstrate that 3D-OCT is a suitable modality for small 
animal imaging studies of muscular dystrophy.
Indocyanine green enhanced near-infrared laser treatment of SCK tumors in a 
mouse model 
Paper 7901-37 of Conference 7901
Date: Monday, 24 January 2011
Time: 3:45 PM – 4:00 PM
Author(s): Gal Shafirstein, Univ. of Arkansas for Medical Sciences (United 
States); Wolfgang Bäumler, Univ. Clinics Regensburg (Germany); Ran Friedman, K. 
Barnes, Leah Hennings, Jessica Weber, Robert Griffin, Univ. of Arkansas for 
Medical Sciences (United States)
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The objective of this study was to determine the efficacy of indocyanine green 
(ICG) dye in enhancing near infrared (NIR) laser ablation of tumors in a mouse 
model. Tumors were treated with 808-nm laser using 86 J/cm2 radiant exposures 
preceded by intravenous injection of 4 mg/kg body weight of ICG solution or 
sterile water. No skin damage was observed in the treated animals. Minor thermal 
damage and necrosis was observed histologically in the tumor post laser/water 
treatment and substantial intra-tumor damage was observed in tissue collected 
from tumors that were treated with laser/ICG.
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Differential distribution of dopamine functionalized quantum rods in mouse 
Paper 7909-43 of Conference 7909
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): A. Guardascione, Istituto di Cibernetica CNR (Italy); A. Ragusa, 
National Nanotechnology Lab. CNR (Italy); M. Rimoli, R. Russo, Univ. Federico II 
(Italy); Claudia Tortiglione, Angela Tino, Istituto di Cibernetica CNR (Italy)
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The conjugation of bioactive molecules to water soluble fluorescent 
semiconductors nanocrystals, opens new perspectives to the studies of drug 
distribution in target tissues and organs. The neurotransmitter dopamine (DA) is 
involved in a variety of signaling pathways and its altered levels have been 
found in different pathological conditions, such as Parkinson's disease and 
attention deficit hyperactivity disorder (ADHD). The possibility to modulate 
brain DA levels might hold great promise for therapeutic purposes. As free DA is 
not able to cross the blood-brain barrier DA based produg, such as 
galactosylated DA, GalDA, already proved to mediate DA diffusion across the BBB. 
With the aim to investigate the extent of their release/accumulation into target 
cells, we have recently produced fluorescent nanocrystals (Quantum Rods) 
conjugated to GalDA. Here, we characterize the pharmacodistribution of the 
functional abduct (GalDA-QRs) administered intravenously in mice. We present the 
selective distribution of GalDA-QRs one hour after injection and the relative 
amount detected ex vivo in different organs is discussed in the general frame of 
cell- and tissue specific interactions with nanoparticles, opening new 
perspectives in the design and feasibility to use inorganic nanoparticles for 
diagnosis and therapeutic purposes.
Imaging of the intact mouse cochlea by spectral-domain optical coherence 
tomography 
Paper 7889-108 of Conference 7889
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Simon S. Gao, Rice Univ. (United States); Anping Xia, Stanford Univ. 
(United States); Tao Yuan, Patrick Raphael, Baylor College of Medicine (United 
States); Ryan L. Shelton, Brian E. Applegate, Texas A&M Univ. (United States); 
John S. Oghalai, Baylor College of Medicine (United States)
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Current medical imaging modalities do not provide high enough resolution to 
detect minor changes in the cochlea, the hearing organ. We sought to develop the 
technique of optical coherence tomography (OCT) to image the cochlea 
noninvasively. We used spectral domain OCT with a center wavelength of 950 nm 
and a bandwidth of ~100 nm. We found that the intracochlear soft tissue is 
visible through bone and that structural differences can be seen in the cochlea 
of newborn and adult mice. We conclude that spectral domain OCT is an effective 
technique for noninvasive imaging of the murine cochlea.
In-vivo cellular metabolism of mouse liver revealed by multiphoton microscopy
Paper 7903-62 of Conference 7903
Date: Tuesday, 25 January 2011
Time: 10:35 AM – 10:50 AM
Author(s): Chun-Chin Wang, Wei-Liang Chen, Zhi-Ru Lin, Feng-Chieh Li, Ara 
Ghazaryan, Hsuan-Shu Lee, Sung-Jan Lin, Chen-Yuan Dong, National Taiwan Univ. 
(Taiwan)
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We performed a novel method to observe the dynamics of the uptake, processing, 
and excretion of fluorescent probes in the hepatobiliary system of mice in vivo. 
A hepatic window was installed on the upper abdomen of mice to acquire 
time-lapse images. The high resolution images show sequential uptake and 
processing of fluorescent probes by hepatocytes and the subsequent excretion 
into bile canaliculi within 50 min. The kinetics of fluorescence intensities in 
hepatocytes and sinusoids were measured and analyzed in time series and spatial 
distribution. We demonstrated a promising technique to study intravital hepatic 
metabolism about normal and diseased mice.
Multimodality optical imaging of ovarian cancer in a post-menopausal mouse model
Paper 7890-32 of Conference 7890
Date: Tuesday, 25 January 2011
Time: 11:30 AM – 11:50 AM
Author(s): Jennifer M. Watson, Photini F. Rice, David L. Bently, Samuel L. 
Marion, The Univ. of Arizona (United States); Molly A. Brewer, Univ. of 
Connecticut Health Ctr. (United States); Patricia B. Hoyer, Jennifer K. Barton, 
The Univ. of Arizona (United States)
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Our goal is to use optical imaging to detect cancer development on the sub 
cellular scale. By determining the microscopic changes that precede ovarian 
cancer we hope to develop a minimally invasive screening test for high risk 
patients. A mouse ovarian cancer model has been developed by treating mice with 
4-Vinylcyclohexene Diepoxide to induce ovarian failure and 7, 
12-Dimethylbenz[a]anthracene (DMBA) to induce ovarian cancer. Using optical 
coherence tomography (OCT) and multiphoton microscopy (MPM) we have obtained 
co-registered en face images of twenty mouse ovaries ex vivo. Preliminary 
analysis indicates that OCT and MPM can visualize ovarian microstructure. During 
the next year we will be completing a long term survival study using 
post-menopausal mice that have been treated with DMBA to induce cancer and 
imaged in vivo at time points before and after treatment.
Fluorescence lifetime molecular tomography of a genetically expressed FRET 
construct in a mouse 
Paper 7896-65 of Conference 7896
Date: Wednesday, 26 January 2011
Time: 9:50 AM – 10:10 AM
Author(s): James A. McGinty, Imperial College London (United Kingdom); Vadim Y. 
Soloviev, Univ. College London (United Kingdom); Daniel W. Stuckey, Khadija B. 
Tahir, Romain Laine, Imperial College London (United Kingdom); Dominic J. Wells, 
The Royal Veterinary College (United Kingdom); Jo V. Hajnal, Alessandro Sardini, 
Imperial College London (United Kingdom); Simon R. Arridge, Univ. College London 
(United Kingdom); Paul M. W. French, Imperial College London (United Kingdom)
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We demonstrate 3-D tomographic FLIM reconstruction of a genetically expressed 
FRET construct, including negative controls, in mice ex vivo. The FRET construct 
and controls were characterised in a time-resolved spectrofluorometer before 
being electroporated into the anterior tibialis of mice. Five days 
post-electroporation, at the peak of expression, the mice were sacrificed and 
imaged, acquiring both excitation and fluorescence signals using a wide-field 
time-gated imaging system with rotational scanning. The reconstructions, using a 
diffusion analogue of a back-projection algorithm, display a reduction in 
fluorescence lifetime and quantum yield for the FRET construct compared to the 
controls, clearly reporting the FRET interaction.
 
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Optical microangiography provides in vivo 3D images of intracochlear 
microstructures and microvascular perfusion in mice 
Paper 7883C-186 of Conference 7883C
Date: Saturday, 22 January 2011
Time: 1:10 PM – 1:30 PM
Author(s): Ruikang K. Wang, Hrebesh M. Subhash, Viviana Davila, Hai Sun, Anh T. 
Nguyen-Huynh, Alfred L. Nuttall, Oregon Health & Science Univ. (United States)
No abstract available Add to My Schedule 
Dynamic three-dimensional imaging of lung parenchyma by OCT in mice 
Paper 7893-24 of Conference 7893
Date: Monday, 24 January 2011
Time: 8:20 AM – 8:40 AM
Author(s): Sven Meissner, Technische Univ. Dresden (Germany); Arata Tabuchi, St. 
Michael's Hospital (Canada); Michael Mertens, Charité Universitätsmedizin Berlin 
(Germany); Wolfgang M. Kübler, St. Michael's Hospital (Canada); Edmund Koch, 
Technische Univ. Dresden (Germany)
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We present a method for dynamic 3-D imaging of healthy and injured subpleural 
lung tissue in the ventilated mouse. We use triggered swept source OCT to image 
murine subpleural alveoli during the inspiratory phase. The acquired B-scans are 
combined off-line into one volume scan for each pressure level. The air fraction 
in healthy lungs and injured lungs is measured using 2-D OCT en-face images. 
Upon lung inspiration from 2 to 12 cmH2O ventilation pressure, the air fraction 
increases in healthy lungs by up to 11% and in injured lungs by 8%. This 
expansion correlates well with results of previous studies.
In-vivo optical measurement of activity-dependent fluorescence change in 
striatum using synaptophluorin mice 
Paper 7883G-140 of Conference 7883G
Date: Monday, 24 January 2011
Time: 8:50 AM – 9:10 AM
Author(s): Sang Beom Jun, Guohong Cui, Xin Jin, Michael D. Pham, Christopher 
Thaler, Steven S. Vogel, National Institutes of Health (United States); Rui 
Costa, Instituto Gulbenkian de Ciência (Portugal); David M. Lovinger, National 
Institutes of Health (United States)
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A novel method is proposed to monitor neural activity in synaptophluorin 
transgenic mice using fiber optics and time-correlated single photon counting. 
Synaptophluorin is a pH-sensitive EGFP derivative that increases fluorescence 
upon exocytosis. The optic fibers and a microelectrode array were assembled and 
implanted into the dorsolateral striatum region of the mice. Anesthesia with 
isoflurane induced the decrease of photon emission/detection as well as the 
decreases of electrical neural activity. In behaving animals, fluorescence was 
transiently increased by an auditory stimulus. These findings indicate that we 
can use in vivo photometry to measure fluorescence changes that report 
physiological changes in brain.
In vivo longitudinal photoacoustic imaging of subcutaneous tumours in mice 
Paper 7899-40 of Conference 7899
Date: Monday, 24 January 2011
Time: 11:30 AM – 11:45 AM
Author(s): Jan G. Laufer, Peter Johnson, Edward Z. Zhang, Barbara Pedley, Paul 
C. Beard, Univ. College London (United Kingdom)
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Photoacoustic tomography provides 3D images of superficial vascular networks 
with high spatial resolution, can be used to visualise the distribution of 
contrast agents, and is therefore suited to the study of the progression and 
treatment of human diseases in small animal models. In vivo photoacoustic images 
of subcutaneous tumours in mice were acquired over several days to monitor 
tumour growth and changes in the vasculature. Through multiwavelength imaging 
and spectral analysis, differences in the oxygenation distribution across the 
tumour were measured. The results suggest that photoacoustic imaging could play 
a role in the development of new antiangiogenic therapies.
Thermal ablation and/or spatially fractionated radiation (GRID) therapy for 
down-staging locally advanced breast cancer 
Paper 7901-39 of Conference 7901
Date: Monday, 24 January 2011
Time: 4:20 PM – 4:35 PM
Author(s): Gal Shafirstein, Robert Griffin, K. Barnes, Jessica Weber, Sunil 
Sharma, Eduardo G. Moros, Univ. of Arkansas for Medical Sciences (United States)
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The purpose of this work was to test our hypothesis that thermal ablation and/or 
spatially fractionated radiation (GRID) therapy can be used for significant 
tumor cytoreduction of locally advanced tumors. Conductive interstitial thermal 
therapy and/or GRID radiotherapy were used to treat Balb/c mice bearing 4T1 
tumors. A 2 to 4-fold reduction in tumor's growth was observed in the treated 
animals in comparison to the control animals. Our preliminary results showed 
that both GRID and CITT could be effective for significant tumor cytoreduction 
in 4T1 tumors implanted in Balb/c mice. Grant support: Winthrop Rockefeller 
Cancer-Institute, Fashion- Footwear Association of New York.
Non-invasive quantification of the metabolic rate of oxygen (MRO2) by 
photoacoustic microscopy: a hyperthermia study of the mouse ear 
Paper 7899-22 of Conference 7899
Date: Sunday, 23 January 2011
Time: 4:00 PM – 4:15 PM
Author(s): Junjie Yao, Konstantin Maslov, Lihong V. Wang, Washington Univ. in 
St. Louis (United States)
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Many diseases, normal decay and physiological functions are closely related to 
alterations in the metabolic rate of oxygen (MRO2). In this study, we 
demonstrate that all the parameters for MRO2 quantification can be 
simultaneously obtained by optical-resolution photoacoustic microscopy (OR-PAM). 
MRO2 of the mouse ear under normothermia (31 ºC skin temperature) and controlled 
systematic hyperthermia (42 ºC skin temperature) was studied. As a result of 
hyperthermia, the MRO2 increased by 28.3 ± 9.4%. The results show that OR-PAM, 
as a single noninvasive imaging modality, is intrinsically suitable for 
quantitative MRO2 measurement in microenvironments.
Implementing label-free microscopy and spectroscopy to study a new mouse model 
of non-alcoholic steatohepatitis 
Paper 7903-91 of Conference 7903
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Iwan W. Schie, UC Davis Medical Ctr. (United States)
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Background: Most common nonalcoholic steatohepatitis (NASH) models in rodents 
are induced by feeding either diet containing high fat/high calorie (HFC) or 
methionine/choline deficient diet (MCD). The former caused overweight, NASH with 
mild insulin resistance; whereas the latter leads to weight loss, steatosis with 
no insulin resistance.Trans-10, cis-12 conjugated linoleic acid (CLA) is a 
positional and geometric isomer of linoleic acid found in partially hydrogenated 
vegetable oils. Controversial findings exit regarding its role in affecting 
lipid metabolism and fat deposition. The aim of the present study is to 
characterize steatosis influenced by CLA-rich diets using Raman spectroscopy and 
coherent anti-Stokes Raman scattering (CARS) microscopy.
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Depth-resolved optical imaging of hemodynamic response within macro- and 
micro-circulatory beds in mouse brain 
Paper 7898-36 of Conference 7898
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Yali Jia, Oregon Health & Science Univ. (United States); Jingyang 
Jiang, Oregon Health & Science Univ. (United States) and Tianjin Univ. (China); 
Zhongwei Zhi, Ruikang K. Wang, Oregon Health & Science Univ. (United States)
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We introduce a hemodynamic imaging system based on optical micro-angiography 
(OMAG) which is capable of resolving and quantifying 3D dynamic blood perfusion 
down to capillary level. By use of a hybrid scanning protocol, this system can 
measure the optical phase shifts caused by fast moving blood cells in 
macro-circulation and slow moving blood cells in micro-circulation. Here, the 
utility of OMAG was demonstrated by monitoring the hemodynamic response to a 
drug administration in mice. Our preliminary results show the potential of OMAG 
in studying neurovascular pathology and as well as in investigating efficacy of 
treatments.
Functional transcranial photoacoustic micro-imaging of mouse cerebrovascular 
cross-section and hemoglobin oxygenation changes during forepaw electrical 
stimulation 
Paper 7899-106 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Lun-De Liao, You-Yin Chen, Chin-Teng Lin, Jyh-Yeong Chang, National 
Chiao Tung Univ. (Taiwan); Meng-Lin Li, National Tsing Hua Univ. (Taiwan)
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In this study, we report on using a 50-MHz functional photoacoustic microscopy 
(PAM) to transcranially image the cross-section and hemoglobin oxygenation (SO2) 
changes of single mouse cortical vessels in response to left forepaw electrical 
stimulation. Three difference levels of the cortical vessels (i.e., with 
different-sized diameters of 350, 120 and 55 um) on activated regions were 
marked to measure their functional cerebrovascular cross-section and SO2 changes 
as a function of time. The averaged vasodilatation observed at the three vessel 
levels was about 18%, 23% 34% upon stimulation, respectively. Moreover, its 
correlation with the electrical stimulation paradigm was also statistically 
analyzed.
Synthesis and characterization of CdHgTe/SiO2 nanoparticles for in-vivo study of 
their dynamic distribution in mouse model 
Paper 7910-26 of Conference 7910
Date: Tuesday, 25 January 2011
Time: 9:30 AM – 9:50 AM
Author(s): Haiyan Chen, Sisi Cui, Yueqing Gu, China Pharmaceutical Univ. (China)
Hide Abstract Add to My Schedule 
In this study, CdHgTe/SiO2 core-shell nanoparticles were synthesized by coating 
of silylating reagent on the surface of CdHgTe QDs. The size change after 
coating a silica shell had been characterized by laser size analyzer. 
Photoluminescence studies showed that the silica shell resulted in a minor 
decline of fluorescence intensity and greatly increased photostability in 
phosphate-buffered saline buffers. Acute toxicity study indicated the obvious 
toxicity reduction of CdHgTe QDs after coating with silica shell. The dynamic 
bio-distribution of CdHgTe/SiO2 nanoparticles in living mouse was in vivo 
monitored by a NIR imaging system. Results indicated the liver-intestine 
metabolic pathway of these Nanoparticles.
Anti-transforming growth factor beta antibody combined with photodynamic therapy 
for renal cell carcinoma in mice 
Paper 7900-2 of Conference 7900
Date: Monday, 24 January 2011
Time: 9:30 AM – 10:00 AM
Author(s): Michael R. Hamblin, Pawel A. Mroz M.D., Massachusetts General 
Hospital (United States)
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Photodynamic therapy (PDT) has been shown to be an effective locally ablative 
anti-cancer treatment that has the additional advantage of inducing 
tumor-directed immune response. We hypothesize that PDT combined with anti-TGF 
beta antibody that does not significantly affect the population of cytotoxic T 
lymphocytes (CTL) and, at the same time, has the potency to decrease the 
immunosuppressive effects of Treg mediated by TGF beta. This hypothesis was 
tested with aTGF-beta antibody combined with BPD-mediated PDT in a BALB/c renal 
cell carcinoma model.
Volumetric in-vivo imaging of intracochlear microstructures and microvascular 
perfusion in mice using high-speed spectral domain optical coherence tomography 
and ultra-high-sensitive optical micro-angiography 
Paper 7889-102 of Conference 7889
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Hrebesh M. Subhash, Viviana Davila, Hai Sun, Anh T. Nguyen-Huynh, 
Alfred L. Nuttall, Ruikang K. Wang, Oregon Health & Science Univ. (United 
States)
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Studying the inner ear microstructures and microvascular dynamics is extremely 
important to understand the cochlear function and to further advance the 
diagnosis, prevention and treatment of many otologic disorders. There is 
considerable interest in developing new methods for in vivo imaging of the 
complex anatomy of the mammalian cochlea and the micro vascular perfusion within 
it for both clinical as well as fundamental studies. In this study, we explored 
the feasibility of high-speed spectral domain optical coherence tomography 
(SD-OCT) and ultra-high sensitive optical microangiography (UHS-OMAG) for 
volumetric in vivo imaging of intracochlear microstructures and microvascular 
perfusion in mice, respectively.
Label-free in-vivo optical micro-angiography imaging of cerebral capillary blood 
flow within meninges and cortex in mice with the skull left intact 
Paper 7889-37 of Conference 7889
Date: Tuesday, 25 January 2011
Time: 11:00 AM – 11:15 AM
Author(s): Yali Jia, Ruikang K. Wang, Oregon Health & Science Univ. (United 
States)
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Optical microangiography (OMAG) is a recently developed label-free imaging 
method capable of producing 3D images of dynamic blood perfusion within 
micro-circulatory tissue beds at an imaging depth up to ~2 mm, with an 
unprecedented imaging sensitivity to the blood flow at ~4 µm/s. In this study, 
we demonstrate the utility of OMAG in imaging the detailed blood flow 
distributions, at a capillary level resolution, within meninges and cortex in 
mice with the cranium left intact. The results indicate that OMAG can be a 
valuable tool for the study of meningeal circulations
Low-coherence wavefront sensing for AO imaging in rodent eyes 
Paper 7885-42 of Conference 7885
Date: Sunday, 23 January 2011
Time: 11:45 AM – 12:00 PM
Author(s): Robert D. Ferguson, Daniel X. Hammer, Mircea Mujat, Nicusor V. 
Iftimia, Niyom Lue, David P. Biss, Ankit H. Patel, Physical Sciences Inc. 
(United States); James D. Akula, Children's Hospital Boston (United States)
Hide Abstract Add to My Schedule 
Rodent models of human eye disease have significantly increased the demand for, 
and the value of, new in vivo animal eye imagers with cellular resolution. The 
small eye of the mouse has the potential to provide the best and brightest 
imaging of any mammal eye, with superior retinal image resolution. However, due 
to the poor optical quality of mouse eyes even high resolution imaging can't 
easily select layers for precision adaptive optics (AO) correction. We describe 
recent progress toward the develop and demonstration a new, compact multimodal 
AO imaging platform optimized for rodent imaging, and novel alternatives to SHWS 
including a low-coherence wavefront sensing (LCWS) techniques.
In-vivo particle image velocimetry of the blood flow using the confocal laser 
scanning microscope 
Paper 7906A-24 of Conference 7906A
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Ho Lee, Wi-Han Kim, SungMin Choi, Cheol-Woo Park, Kyungpook National 
Univ. (Korea, Republic of)
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In the previous meeting (PhotonicWest 2010), we reported "the blood cell-based 
Particle Image Velocimetry (PIV)" in a micro-tube using the confocal microscope. 
In that study, we employed blood cells as tracing particles, while previous 
microscopy-assisted PIV required exogenous particles as the tracing particles. 
In this study, we are reporting the application of the "the blood cell-based 
PIV" for the measurements of blood stream in a live animal. We used video-rate 
CLSM to observe blood cells in a live mouse ear. The acquired images were used 
to perform PIV, thus providing the blood velocity profile in capillaries of live 
mouse ear.
Steroid-induced osteoporosis monitored by Raman spectroscopy 
Paper 7883F-124 of Conference 7883F
Date: Saturday, 22 January 2011
Time: 9:20 AM – 9:40 AM
Author(s): Jason R. Maher, Masahiko Takahata, Hani A. Awad, Andrew J. Berger, 
Univ. of Rochester (United States)
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Glucocorticoids are frequently used to treat inflammatory disorders such as 
rheumatoid arthritis. Unfortunately, extended exposure to this steroid is the 
leading cause of physician-induced osteoporosis, leaving patients susceptible to 
fractures at rates of 30-50%. In this presentation, we report correlations 
between Raman spectra and biomechanical strength tests on bones of placebo- and 
glucocorticoid-treated mice. Both wild-type mice and a transgenic model of 
rheumatoid arthritis have been studied. A two-way ANOVA model reveals 
statistically significant spectral differences as influenced by glucocorticoid 
treatment and mouse type. In addition, we discuss strategies to extract key 
Raman parameters of bone through overlying soft tissue.
Potentialities of a new bimodal x-ray/fluorescence tomograph within a cyindrical 
geometry for preclinical studies 
Paper 7892-18 of Conference 7892
Date: Saturday, 22 January 2011
Time: 4:40 PM – 5:00 PM
Author(s): Anne Koenig, Anne Planat-Chrétien, Jean-Guillaume Coutard, Lionel 
Hervé, Marco Brambilla, Commissariat à l'Énergie Atomique (France); Véronique 
Josserand, Jean-Luc Coll, Institut Albert Bonniot (France); Jean-Marc Dinten, 
Commissariat à l'Énergie Atomique (France)
Hide Abstract Add to My Schedule 
An instrument dedicated to the co-registration of optical and X-ray 
measurements, has been developed: specific acquisition protocol and 
reconstruction software have been developed for carrying out fluorescence 
diffuse optical tomography in a cylindrical geometry consistent with XCT. Actual 
animal geometry provided by the X-ray tomography is used to give animal 
boundaries to the diffuse optical tomography reconstruction algorithm. To 
evaluate performances of this new optical imaging system, experiments have been 
conducted on phantoms, mice with fluorescent capillaries, and finally on mice 
bearing tumours. The fluorescence reconstructions are shown to be geometrically 
consistent with X-ray ones.
High-resolution in-vivo targeted imaging of colorectal dysplasia with a 
LED-based confocal microendoscope 
Paper 7893-5 of Conference 7893
Date: Sunday, 23 January 2011
Time: 9:30 AM – 9:50 AM
Author(s): Sakib F. Elahi, Sharon J. Miller, Thomas D. Wang M.D., Univ. of 
Michigan (United States)
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We demonstrate a LED-based, flexible, fibered microscope that is sufficiently 
small to pass through the instrument channel of a small animal endoscope for in 
vivo molecular imaging of the colonic mucosa of mice. The instrument delivers 
excitation light through a fiber-optic bundle with outer diameter 680 µm, and 
achieves 0.7 mW of power with a lateral resolution of 4 µm. Independently, 
FITC-labeled selective and control peptides are applied topically to the mucosa 
of transgenic mice that spontaneously develop distal colonic adenomas. Using the 
microendoscope, we found that targeted peptide preferentially binds to adenomas 
with three-fold greater affinity.
In-vivo small animal optical imaging enhanced with indocyanine green and saline
Paper 7892-38 of Conference 7892
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Ning Liu, Yuting Lin, Mitchell Hsing, Orhan Nalcioglu, Gultekin 
Gulsen, Univ. of California, Irvine (United States)
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We present a comparison of the in vivo mice optical images enhanced with ICG and 
saline separately. The multimodality imaging system used here combines 
frequency-domain optical techniques and MRI. 16 fibers (8 illuminations and 8 
collections) radially arranged to obtain the transverse images of the mice 
revealing tumor. The acquisition time for one optical image was 16 seconds. Each 
dynamic measurement lasted for 50 minutes, with bolus injection at 5mins. The 
pharmacokinetics of ICG and saline at the same tumor location showed comparable 
signal level, but opposite curvature variation. The reconstructed tomograms 
showed enhancement at tumor location in both cases.
Systemic induction of heat shock protein 70 following tumor treatment by 
photodynamic therapy 
Paper 7900-1 of Conference 7900
Date: Monday, 24 January 2011
Time: 9:00 AM – 9:30 AM
Author(s): Mladen Korbelik, Soroush Merchant, The BC Cancer Agency Research Ctr. 
(Canada)
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Photodynamic therapy (PDT) induces a strong upregulation of heat shock protein 
70 (Hsp70) in treated tumor. We report that Hsp70 gene expression was increased 
following PDT in the tumor and liver of host mice. Recombinant Hsp70 protein 
administered to tumor-bearing mice accumulated in both the liver and tumor but 
the tumor:liver ratio was found to increase when the tumors were treated by PDT. 
Thus following PDT, Hsp70 is upregulated at distant systemic sites and 
sequestered to damaged tumor tissue to facilitate the disposal of dying cells 
and influence the development of antitumor immune response elicited by this 
therapy.
Monitoring early tumor response to drug therapy using optical tomography 
Paper 7896-43 of Conference 7896
Date: Tuesday, 25 January 2011
Time: 9:10 AM – 9:30 AM
Author(s): Molly L. Flexman, Hyun-Keol Kim, Columbia Univ. (United States); 
Sonia L. Hernandez, Jianzhong Huang, Tessa Johung, Columbia Univ. Medical Ctr. 
(United States); Jong Hwan Lee, Fotios Vlachos, Columbia Univ. (United States); 
Darrell J. Yamashiro, Jessica J. Kandel, Columbia Univ. Medical Ctr. (United 
States); Andreas H. Hielscher, Columbia Univ. (United States)
Hide Abstract Add to My Schedule 
Anti-angiogenic drugs have shown promising results in cancer therapy but have 
also shown a large variability in effectiveness. We present a study that uses 
optical tomography to image mice implanted with two different kidney tumor 
models. We found that a Ewing sarcoma tumor model shows a statistically 
significant drop in blood volume within 5 days of treatment with bevacizumab, an 
FDA approved anti-angiogenic drug. Mice implanted with a neuroblastoma tumor 
model, known to not respond well to bevacizumab, do not show this drop in blood 
volume, suggesting that optical tomographic imaging may be used to monitor early 
treatment response.
Tumor hypoxia fluorescence imaging using 2-nitroimidazole bis-carboxylic acid 
indocyanine dye conjugate 
Paper 7896-63 of Conference 7896
Date: Wednesday, 26 January 2011
Time: 9:10 AM – 9:30 AM
Author(s): Nrusingh C. Biswal, Christopher Pavlik, Michael B. Smith, Univ. of 
Connecticut (United States); Liisa T. Kuhn, Kevin P. Claffey, Univ. of 
Connecticut Health Ctr. (United States); Quing Zhu, Univ. of Connecticut (United 
States)
Hide Abstract Add to My Schedule 
We present the tumor-targeted hypoxia fluorescence imaging using a novel 
2-nitroimidazole indocyanine dye conjugate. In-vivo tumor targeting in six mice 
demonstrated that a measured half-life of 2-nitroimidazole-indocyanine dye wash 
out was significantly longer (112±32.37 minutes) than that of unconjugated 
indocyanine dye alone (69.75±14.01 minutes). Fluorescence images of mice tumors 
showed a 2.6-fold contrast of dye uptake with hypoxic conjugate injection 
compared to that with unconjugated indocyanine dye injection. A fluorescence 
emission ratio of 2.5-fold was found between the tumor cells treated with the 
2-nitroimidazole-indocyanine dye and incubated under hypoxia compared to the 
cells in normoxia condition.
Multisite and multidepth tumors localization enhancement after autofluorescence 
removal 
Paper 7896-64 of Conference 7896
Date: Wednesday, 26 January 2011
Time: 9:30 AM – 9:50 AM
Author(s): Anne-Sophie Montcuquet, Fabrice P. Navarro, Lionel Hervé, 
Commissariat à l'Énergie Atomique (France); Jérôme I. Mars, Institut National 
Polytechnique de Grenoble (France); Jean-Marc Dinten, Commissariat à l'Énergie 
Atomique (France)
Hide Abstract Add to My Schedule 
Fluorescence imaging in diffusive media locates tumors tagged by injected 
fluorescent markers in NIR wavelengths. For deep embedded markers, natural 
autofluorescence of tissues comes to be a limiting factor to tumor detection and 
accurate FDOT reconstructions. A spectroscopic approach coupled with 
Non-negative Matrix Factorization source separation method is explored to 
discriminate fluorescence sources according to their fluorescence spectra and 
remove unwanted autofluorescence. We successfully removed autofluorescence from 
acquisitions on living mice with a single subcutaneous tumor or two capillary 
tubes inserted at different depths. Future experiments on mice with mutli-site 
and multi-depth tumors will be presented at BIOS 2011 symposium.
Using Raman spectroscopy to study the onset of labor 
Paper 7890-45 of Conference 7890
Date: Tuesday, 25 January 2011
Time: 4:50 PM – 5:10 PM
Author(s): Elizabeth Vargis, Nathan Webb, B. C. Paria, Jeff Reese, Kelly 
Bennett, Vanderbilt Univ. (United States); Ayman Al-Hendy, Meharry Medical 
College (United States); Anita Mahadevan-Jansen, Vanderbilt Univ. (United 
States)
Hide Abstract Add to My Schedule 
Preterm labor is the second leading cause of neonatal mortality and can lead to 
a number of complications for the mother and her child. Having a tool to predict 
preterm labor could lead to an increased amount of births that come to term. 
While there are few ways to predict preterm labor with fetal fibronectin 
screening and cervical length measurements, over half of all preterm births are 
not diagnosed and do not fall into any high-risk category. This study seeks to 
predict the onset of labor by using Raman spectroscopy to detect changes in the 
cervix during pregnancy. Raman spectra were acquired from the cervix of 
non-gravid and gravid mice and humans, all of whom delivered at full term. We 
believe significant changes will occur in the Raman spectra obtained during the 
course of pregnancy. Preliminary results show that there are differences based 
on cycling status alone, in both mice and humans. Furthermore, there are 
significant changes that occur during pregnancy. This study will determine if 
Raman spectroscopy can be used to predict when labor will occur, most likely due 
to the effect of cervical softening and changes in hormonal levels on the 
spectra. Any algorithm that can be developed to predict when a woman will enter 
labor will greatly benefit the outcome for pregnant women and their children.
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Kinetics of gold nanorod distribution in mouse tissues after intravenous 
injection monitored with optoacoustic tomography 
Paper 7899-157 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Richard Su, Anton Liopo, Hans-Peter F. Brecht, Sergey A. Ermilov, 
Alexander A. Oraevsky, TomoWave Labs., Inc. (United States)
Hide Abstract Add to My Schedule 
A three dimensional laser optoacoustic imaging system analyzed the kinetics of 
gold nanorod (GNR) distribution after being intravenously injected into live 
mice. Animals were scanned prior to GNR injection and then periodically up to 
one week post-injection. Because GNR were stabilized with a toxic material, 
cetyltrimethylammonium bromide, we purified GNR for in vivo use by 
centrifugation, filtration, and pegylation and verified in MTT assays. Higher 
levels of GNR were found in liver macrophages after 48 hours and decreased after 
seven days. GNR injected in mice were found in the periphery within hours before 
settling into certain organs after a day.
Folate receptor targeted Type-1 photosensitizer bioconjugates for tumor 
visualization and phototherapy 
Paper 7886-12 of Conference 7886
Date: Saturday, 22 January 2011
Time: 3:30 PM – 3:50 PM
Author(s): Raghavan Rajagopalan, Amruta R. Poreddy, Nicole Putnam, Amolkumar 
Karwa, Rick M. Fitch, Karen P. Galen, Maureen Nichols, Lori Chinen, Arti Naik, 
Carolyn Sympson, Richard B. Dorshow, Covidien (United States)
Hide Abstract Add to My Schedule 
Folate receptors are over expressed in many types of cancers, including, 
ovarian, breast, and cervical. In our continuing efforts toward the development 
of targeted Type 1 phototherapeutic agents, an azide-based Type 1 
photosensitizer, a fluorophore, and a dual diagnostic-therapeutic probe 
consisting of the fluorophore and the photosensitizer units were prepared and 
independently conjugated to two vectors that target folate receptors. The 
results of in vitro binding and cell viability assays using KB ovarian cancer 
cells, and in vivo studies using the nude mouse xenograft model demonstrating 
selective uptake and tumor destruction will be presented.
Simultaneous multimodality optical and MR imaging of tumor micro-environment 
within implanted window chambers 
Paper 7902-14 of Conference 7902
Date: Saturday, 22 January 2011
Time: 4:15 PM – 4:35 PM
Author(s): Mir Farrokh Shayegan Salek, College of Optical Sciences, The Univ. of 
Arizona (United States); Dominique Jennings, Harvard-Massachusetts Institute of 
Technology (United States); Tzu-Yu Wu, Arthur F. Gmitro, The Univ. of Arizona 
(United States)
Hide Abstract Add to My Schedule 
A modular platform capable of doing optical microscopy inside an MRI instrument 
is developed. This is done by relaying the optical image to outside of the MR 
bore. Our device enables simultaneous optical and MR imaging of the same tissue 
and thus creates the ideal situation for doing comparative or complementary 
studies using these two modalities. Initial experiments have been done using GFP 
labeled tumor cells implanted in mouse dorsal skin fold window chamber. Overall 
system design and results of preliminary vascular permeability studies will be 
presented.
High-speed dynamic laser speckle imaging of changes of microcirculation in vivo
Paper 7898-11 of Conference 7898
Date: Sunday, 23 January 2011
Time: 9:50 AM – 10:10 AM
Author(s): Jia Qin, Lin An, Ruikang K. Wang, Oregon Health & Science Univ. 
(United States)
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In this study, we will present our novel observations when a high speed laser 
speckle imaging method is used to image the microcirculation within tissue beds. 
Based on these new observations, we demonstrate the relative changes of dynamic 
microvascular blood flow through occluding the main blood vessels and then 
reperfusion in the mouse ear flap. The promising results show that the high 
speed LSI can give useful information as to transient and dynamic 
microcirculation during occlusion and reperfusion.
Smart velocity ranging quantifiable optical micro-angiography 
Paper 7898-18 of Conference 7898
Date: Sunday, 23 January 2011
Time: 2:20 PM – 2:40 PM
Author(s): Zhongwei Zhi, Yali Jia, Lin An, Ruikang K. Wang, Oregon Health & 
Science Univ. (United States)
Hide Abstract Add to My Schedule 
In this study, we introduce a new type of OMAG called Quantifiable Optical 
Microangiography (QOMAG) which is capable of performing quantitative flow 
imaging with smart velocity ranging. The feasibility of QOMAG for quantitative 
flow imaging is evaluated using a well defined flow in a glass capillary. 
Further, in vivo studies were executed on cerebral blood flow of mouse model 
with the cranium left intact. Multi-range detailed blood flow velocity 
distribution within intracranial dura mater and cortex can be given by QOMAG 
simultaneously.
In vivo skin microscopy 
Paper 7893-4 of Conference 7893
Date: Monday, 24 January 2011
Time: 3:00 PM – 3:20 PM
Author(s): Wibool Piyawattanametha, National Electronics and Computer Technology 
Ctr. (Thailand); Hyejun Ra, Emilio Gonzalez-Gonzalez, Stanford Univ. School of 
Medicine (United States); Michael J. Mandella, National Electronics and Computer 
Technology Ctr. (Thailand); Gordon S. Kino, Stanford Univ. School of Medicine 
(United States); Olav D. Solgaard, National Electronics and Computer Technology 
Ctr. (Thailand); Devin Leake, Dharmacon, Inc. (United States); Thomas D. Wang 
M.D., Univ. of Michigan (United States); Roger L. Kaspar, TransDerm, Inc. 
(United States); Anthony Oro, Christopher H. Contag, Stanford Univ. School of 
Medicine (United States)
Hide Abstract Add to My Schedule 
We demonstrate a Dual-Axes Confocal (DAC) fluorescence microscopy and obtain in 
vivo skin images in mouse models and humans. The DAC microscope delivers an 
excitation wavelength of 785 nm with a maximum laser output of 2.5 mW at the 
surface mucosa. Confocal images can then be collected at a scan rate of 5 
frames/second. The transverse and axial resolutions are 5 µm and 7 µm, 
respectively.
In vivo skin microscopy 
Paper 7930-4 of Conference 7930
Date: Monday, 24 January 2011
Time: 3:00 PM – 3:20 PM
Author(s): Wibool Piyawattanametha, National Electronics and Computer Technology 
Ctr. (Thailand); Hyejun Ra, Emilio Gonzalez-Gonzalez, Stanford Univ. School of 
Medicine (United States); Michael J. Mandella, National Electronics and Computer 
Technology Ctr. (Thailand); Gordon S. Kino, Stanford Univ. School of Medicine 
(United States); Olav D. Solgaard, National Electronics and Computer Technology 
Ctr. (Thailand); Devin Leake, Dharmacon, Inc. (United States); Thomas D. Wang 
M.D., Univ. of Michigan (United States); Roger L. Kaspar, TransDerm, Inc. 
(United States); Anthony Oro, Christopher H. Contag, Stanford Univ. School of 
Medicine (United States)
Hide Abstract Add to My Schedule 
We demonstrate a Dual-Axes Confocal (DAC) fluorescence microscopy and obtain in 
vivo skin images in mouse models and humans. The DAC microscope delivers an 
excitation wavelength of 785 nm with a maximum laser output of 2.5 mW at the 
surface mucosa. Confocal images can then be collected at a scan rate of 5 
frames/second. The transverse and axial resolutions are 5 µm and 7 µm, 
respectively.
A combined photoacoustic, pulse echo ultrasound and optical coherence tomography 
endoscopy 
Paper 7899-158 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Yi Yang, Tianheng Wang, Patrick D. Kumavor, Univ. of Connecticut 
(United States); Xiang Li, Qifa Zhou, The Univ. of Southern California (United 
States); Quing Zhu, Univ. of Connecticut (United States)
Hide Abstract Add to My Schedule 
We have developed a novel prototype combined photoacoustic, pulse-echo 
ultrasound and OCT endoscopy. The endoscopy consists of a ball lensed OCT probe, 
a right-angle multimode fiber for delivering the laser beam for PAT, and a high 
frequency ultrasound transducer of 35 MHz center frequency. Mouse ear and pig 
ovary were imaged ex vivo to demonstrate the capability of this new combined 
endoscopy. Simultaneously acquired microvascular and high resolution anatomy 
images at subsurface and deeper tissue range demonstrate the synergy of the 
combined endoscopy over each modality alone.
Tracking Au nanoring delivery into biotissue with optical coherence tomography
Paper 7889-114 of Conference 7889
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Cheng-Kuang Lee, Hung-Yu Tseng, Chia-Yun Lee, Han-Yi Chou, Shou-Yen 
Wu, Ting-Ta Chi, Kai-Min Yang, Jyh-Yang Wang, Yean-Woei Kiang, Chih-Chung Yang, 
National Taiwan Univ. (Taiwan); Meng-Tsan Tsai, Chang Gung Univ. (Taiwan)
Hide Abstract Add to My Schedule 
The resonant and non-resonant Au nanorings (NRIs) are delivered into mouse liver 
samples for tracking their diffusion in the samples through continual optical 
coherence tomography (OCT) scanning for one hour. With resonant Au NRIs, the 
average A-mode scan profiles of OCT scanning at different delay times clearly 
demonstrate the extension of strong backscattering depth with time. The 
calculation of speckle variance among successive OCT scanning images, which can 
be used to represent the local transport speed of Au NRIs, leads to the 
illustrations of downward propagation and spreading of major Au NRI motion spot 
with time.
In-vivo cancer therapy monitoring with diffuse optical techniques 
Paper 7896-41 of Conference 7896
Date: Tuesday, 25 January 2011
Time: 8:30 AM – 8:50 AM
Author(s): Regine Choe, Saurav Pathak, So Hyun Chung, Univ. of Pennsylvania 
(United States); Turgut Durduran, ICFO - Instituto de Ciencias Fotónicas 
(Spain); Han Y. Ban, David R. Busch, Tiffany Averna, Erin M. Buckley, Meeri N. 
Kim, Univ. of Pennsylvania (United States); Angela DeMichele, Carolyn Mies, Mark 
A. Rosen, Mitchell D. Schnall, The Univ. of Pennsylvania Health System (United 
States); Arjun G. Yodh, Univ. of Pennsylvania (United States)
Hide Abstract Add to My Schedule 
There is a great interest in detecting early metabolic changes which may precede 
morphological changes. To this end, we measured blood flow, oxy- and 
deoxy-hemoglobin concentrations of cancer using a hybrid frequency-domain 
diffuse optical and correlation spectroscopy instrument to track therapy. The 
results of monitoring neoadjuvant chemotherapy of breast cancer patients in 
correlation to histopathological response will be presented. In addition, the 
effects of radiation therapy in human head and neck patients, and molecular 
therapy on a xenograft mouse model of head and neck cancer will be presented.
Fluorescence lifetime optical projection tomography 
Paper 7904-19 of Conference 7904
Date: Tuesday, 25 January 2011
Time: 4:50 PM – 5:10 PM
Author(s): James A. McGinty, Imperial College London (United Kingdom); Daniel W. 
Stuckey, Imperial College Healthcare NHS Trust (United Kingdom); Gao Sun, 
Harriet B. Taylor, Guy A. Rutter, Imperial College London (United Kingdom); 
Alessandro Sardini, Imperial College Healthcare NHS Trust (United Kingdom); 
Jonathan R. Lamb, Imperial College London (United Kingdom); Gordon W. Stamp, The 
Royal Marsden NHS Foundation Trust (United Kingdom); Margaret J. Dallman, Paul 
M. W. French, Imperial College London (United Kingdom)
Hide Abstract Add to My Schedule 
Having extended optical projection tomography (OPT) to 3-D fluorescence lifetime 
tomography (tomoFLIM), we present a detailed characterisation of an 
intensity-based and time-resolved OPT system that we have optimised in terms of 
spatial resolution, signal-to-noise and total acquisition time. This system has 
been applied to cm scale volumetric imaging of chick embryos, mouse pancreas (to 
measure the islet volume in excised murine pancreata) and human tissue 
resections (for 3-D histology without the need for serial sectioning). We have 
also developed a higher magnification system implementing modulation transfer 
function-dependent filters for imaging zebrafish expressing fluorescent protein 
labels.
Ultra-high-sensitive optical micro-angiography reveals dynamic changes of 
depth-resolved microcirculations within skeletal muscles 
Paper 7898-2 of Conference 7898
Date: Saturday, 22 January 2011
Time: 1:30 PM – 2:00 PM
Author(s): Yali Jia, Ruikang K. Wang, Oregon Health & Science Univ. (United 
States)
Hide Abstract Add to My Schedule 
In this study, we demonstrate the utility of OMAG in imaging the detailed blood 
flow distributions, at a capillary level resolution, within skeletal muscles in 
mice. By use of the mouse model of hind-limb ischemia, we show OMAG can yield 
the chronic assessment of time-dependent changes in muscle perfusion and 
perfusion reserve along tissue depth. These findings indicate that OMAG can 
represent a sensitive and consistent technique to effectively study 
pharmacologic therapies aimed at promoting the growth and development of 
collateral vessels.
Validation of method for enhanced production of red-shifted bioluminescent 
photons in vivo 
Paper 7902-33 of Conference 7902
Date: Sunday, 23 January 2011
Time: 4:00 PM – 4:20 PM
Author(s): Joe Dragavon, Samantha Blazquez, Chelsea Samson, Spencer Shorte, 
Institut Pasteur (France)
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Bioluminescence imaging is a technique that allows for the non-invasive 
observation of biological events in intact living organisms, ranging from single 
cells to small rodents. In animal models, the constant presence of hemoglobin 
leads to a further decrease in detectable photons. We have developed and 
validated a technique that is able to red-shift the bioluminescent photons to 
the optical region of >650nm, a region of minimal absorbance by hemoglobin. We 
show this novel technique yields a substantial increase in the number of red 
photons for in vitro and in vivo conditions, both in isolated single cells and 
intact living mice
Bioconjugated ICG-micellar nanocapsules as translational fluorescent agents for 
in-vivo optical molecular imaging 
Paper 7910-25 of Conference 7910
Date: Tuesday, 25 January 2011
Time: 9:10 AM – 9:30 AM
Author(s): Yong-Ping Chen, The Johns Hopkins Univ. (United States); Kyle L. 
Davis, North Carolina State Univ. (United States); Michelle Garner, Tulane Univ. 
(United States); Xingde Li, The Johns Hopkins Univ. (United States)
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To enable bioconjugation for tumor targeting and molecular imaging, the (PEO)-OH 
terminals on the corona of the ICG-micelles are pre-activated and then 
conjugated with antibodies. Recently in vivo fluorescence imaging of 
tumor-bearing mice with bioconjugated ICG-micelles has demonstrated strong 
enhancement in molecular specificity when comparing with nonconjugated 
ICG-micelles or free ICG. The bio-functionalized ICG-nanocapsules hold strong 
promise for translating optical molecular imaging to in vivo clinical practice.
Imaging sub-nanomolar concentrations through more than five centimeters of 
tissue with time-domain diffuse fluorescence tomography 
Paper 7896-66 of Conference 7896
Date: Wednesday, 26 January 2011
Time: 10:40 AM – 11:00 AM
Author(s): Frederic Leblond, Fadi El-Ghussein, Brian W. Pogue, Dartmouth College 
(United States); Kenneth M. Tichauer, Dartmouth College (Canada); Robert W. 
Holt, Dartmouth College (United States)
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Photodetection based on time-correlated single-photon counting technology is 
used to demonstrate that diffuse fluorescence tomography can detect fluorophores 
in transmission through more than five centimeters in tissue-simulating 
phantoms, and that this can be achieved for sub-nanomolar concentrations with 
dyes commonly used for in vivo pre-clinical biological studies. Our results 
demonstrate that an unprecedented level of sensitivity can be achieved with 
time-domain fluorescence tomography allowing this technology to be used for 
applications involving animals larger than mice as well as applications where 
limited contrast is available.
Quantitative in-vivo lifetime imaging using a time-domain platform with a 
supercontinuum tunable laser for extended spectral coverage 
Paper 7910-54 of Conference 7910
Date: Wednesday, 26 January 2011
Time: 1:50 PM – 2:10 PM
Author(s): Niculae Mincu, Dao Chao Huang, Marilyse Piche, Guobin Ma, Advanced 
Research Technologies Inc. (Canada)
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The continuously expanding number of fluorescent probes developed for molecular 
imaging in vivo requires new instruments, more flexible and with higher 
quantification power. Responding to those requirements we propose a new 
instrument: it combines the sensitivity of time correlated single photon 
detection with the extended spectral coverage of a pulsed supercontinuum laser 
in a sensitive and flexible time-domain platform for in vivo molecular imaging 
in small animals. The performance of the system is demonstrated on a case study, 
using NEO-STEM-PMSR50-PEG fluorescent nanoprobes and sequential imaging of CD-1 
nude mice.
Nanoscale nuclear architecture for cancer diagnosis by spatial-domain 
low-coherence quantitative phase microscopy 
Paper 7907-3 of Conference 7907
Date: Saturday, 22 January 2011
Time: 9:10 AM – 9:30 AM
Author(s): Pin Wang, Rajan K. Bista, David Y. Lo, Walid E. Khalbuss, Wei Qiu, 
Kevin D. Staton, Lin Zhang, Univ. of Pittsburgh (United States); Teresa A. 
Brentnall M.D., Univ. of Washington (United States); Randall E. Brand M.D., Yang 
Liu, Univ. of Pittsburgh (United States)
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Alterations in nuclear architecture are the hallmark diagnostic characteristic 
of cancer cells. In this work, we show that the nuclear architectural 
characteristics quantified by spatial-domain low-coherence quantitative phase 
microscopy (SL-QPM), is more sensitive for the identification of cancer cells 
than conventional cytopathology. We demonstrated the importance of nuclear 
architectural characteristics in both an animal model of intestinal 
carcinogenesis - APC/Min mouse model and human cytology specimens with 
colorectal and pancreatic cancers by identifying cancer from cytologically 
non-cancerous appearing cells. The determination of nanoscale nuclear 
architecture using this simple and practical optical instrument is a significant 
advance towards cancer diagnosis.
Long-term, time-lapse, multimodal microscopy for tracking cell dynamics in live 
tissue 
Paper 7902-4 of Conference 7902
Date: Saturday, 22 January 2011
Time: 9:30 AM – 9:50 AM
Author(s): Benedikt W. Graf, Eric J. Chaney, Maria Carmen Valero Quiros, Marina 
Marjanovic, Marni D. Boppart, Stephen A. Boppart M.D., Univ. of Illinois at 
Urbana-Champaign (United States)
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High speed intravital microscopy has emerged as an essential tool for studying 
cellular dynamics in live tissue. However the timescales that tissue can be 
continuously observed is limited to several hours. We present methods for 
observing long term cellular dynamics in live tissue based on three-dimensional 
registration of time-lapse intravital microscopy images. These methods are 
applied for in vivo tracking of bone-marrow derived GFP-labeled stem cells in 
mouse skin following bone marrow transplants from GFP donors into wildtype 
hosts. This enables tracking of these cells after local cutaneous injury, and 
for investigating the role of skin stem cells in wound healing.
Monitoring human melanocytic cell responses to piperine using multispectral 
imaging 
Paper 7883A-8 of Conference 7883A
Date: Saturday, 22 January 2011
Time: 10:50 AM – 11:10 AM
Author(s): Ravikant Samatham, Kevin G. Phillips, Julia Sonka, Philippe 
Thuillier, Amala Soumyanath, Steven L. Jacques, Oregon Health & Science Univ. 
(United States)
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Vitiligo is a depigmentary disease characterized by melanocyte loss attributed 
most commonly to autoimmune mechanisms. Piperine, a compound found in black 
pepper, is a potential treatment for the depigmentary skin disease vitiligo, due 
to its ability to stimulate mouse epidermal melanocyte proliferation in vitro 
and in vivo. The present study investigates the use of multispectral imaging to 
quantify the stimulatory effects of piperine on human melanocyte proliferation 
in reconstructed epidermis. We find a direct link between increased absorption 
due to melanin in multispectral imaging and increased melanocyte proliferation 
and dendritic spread revealed by standard bright field microscopy.
Wide-field in-vivo spectral and fluorescence imaging microscopy of microvessel 
blood supply and oxygenation 
Paper 7902-7 of Conference 7902
Date: Saturday, 22 January 2011
Time: 11:45 AM – 12:05 PM
Author(s): Jennifer Lee, Mamta Wankhede, Brian S. Sorg, Univ. of Florida (United 
States)
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The ability to measure microvessel function in laboratory animals can be useful 
for development of vascular targeting drugs. Blood supply time gives information 
related to microvessel morphology and hemoglobin saturation gives information on 
microvessel oxygen transport. These parameters together may yield much 
information since theoretically microvessel morphology can influence microvessel 
oxygenation in some tissues; however, these measurements have not yet been 
combined. In this study, we report the combination of blood supply time and 
hemoglobin saturation imaging of microvessels in tumors using widefield 
fluorescence and spectral imaging, respectively. The correlation between the 
measurements in a mouse mammary tumor is analyzed.
Size- and structure-dependent toxicity of silica particulates 
Paper 7909-9 of Conference 7909
Date: Saturday, 22 January 2011
Time: 1:55 PM – 2:05 PM
Author(s): Sanshiro Hanada, Kenichi Miyaoi, Akiyoshi Hoshino, Kenji Yamamoto 
M.D., International Medical Ctr. of Japan (Japan)
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Nano- and micro-particulates firmly attach with the surface of various 
biological systems. In some chronic pulmonary disease such as asbestosis and 
silicosis, causative particulates will induce chronic inflammatory disorder, 
followed by poor prognosis diseases. We assessed cytotoxicity of the various 
kinds of silica particles, including amorphous and crystal silica, in mouse 
alveolar macrophage culture. Their cytotoxicity depends on particle size and is 
related with inflammation response. By contrast, production of TGF-beta, which 
is fibrosis maker, by addition of crystal silica was much higher than that of 
amorphous silica. We conclude that differences of silica particulate affect 
cytotoxicity and immune response.
Fully parallel adaptive finite element simulation using the simplified spherical 
harmonics approximations for frequency domain fluorescence molecular imaging 
Paper 7892-14 of Conference 7892
Date: Saturday, 22 January 2011
Time: 2:40 PM – 3:00 PM
Author(s): Yujie Lu, Banghe Zhu, The Univ. of Texas Health Science Ctr. at 
Houston (United States); Haiou Shen, Virginia Polytechnic Institute and State 
Univ. (United States); John C. Rasmussen, The Univ. of Texas Health Science Ctr. 
at Houston (United States); Ge Wang, Virginia Polytechnic Institute and State 
Univ. (United States); Eva M. Sevick-Muraca, The Univ. of Texas Health Science 
Ctr. at Houston (United States)
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In frequency-domain fluorescence molecular imaging, diffusion approximation 
theory has been extensively applied. However, high-order photon migration models 
need to be further investigated. In this paper, a frequency-domain parallel 
adaptive finite element solver is developed with the simplified spherical 
harmonics (SPN) approximations. The validation results show that high-order SPN 
can effectively correct the modeling errors of diffusion equation especially 
when the tissues have high absorption characteristics and/or when high 
modulation frequency measurements are used. Furthermore, the parallel adaptive 
mesh evolution strategy improves the modeling precision and the simulation speed 
on a realistic digital mouse phantom.
Localized surface plasmon properties of Au nanorings and their diffusion in 
biotissue 
Paper 7909-15 of Conference 7909
Date: Saturday, 22 January 2011
Time: 5:05 PM – 5:25 PM
Author(s): Cheng-Kuang Lee, Shou-Yen Wu, Hung-Yu Tseng, Ting-Ta Chi, Kai-Min 
Yang, Jyh-Yang Wang, National Taiwan Univ. (Taiwan); Meng-Tsan Tsai, Chang Gung 
Univ. (Taiwan); Yean-Woei Kiang, Chih-Chung Yang, National Taiwan Univ. (Taiwan)
Hide Abstract Add to My Schedule 
Aqueous solutions of Au nanorings (NRs) with different localized surface plasmon 
resonance (LSPR) wavelengths are prepared. The resonant and non-resonant Au NRs 
are delivered into mouse liver samples for tracking Au NR diffusion through OCT 
scanning. With resonant Au NRs, the average A-mode scan profiles of OCT scanning 
at different delay times demonstrate the extension of strong backscattering 
depth. The calculation of speckle variance among successive OCT scanning images, 
which can be used to represent the local transport speed of Au NRs, leads to the 
illustrations of downward propagation and spreading of major Au NR motion spot 
with time.
Endoscopic detection of murine colonic dysplasia using a novel fluorescently 
labeled peptide 
Paper 7893-2 of Conference 7893
Date: Sunday, 23 January 2011
Time: 8:30 AM – 8:50 AM
Author(s): Sharon J. Miller, Bishnu Joshi, Adam Gaustad, Eric R. Fearon, Thomas 
D. Wang M.D., Univ. of Michigan (United States)
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Current screening endoscopy does not detect all pre-malignant (dysplastic) 
colorectal mucosa, thus requiring the development of more sensitive, targeted 
techniques to improve detection. The presented work utilized phage display to 
identify a novel peptide binder to colorectal dysplasia in a CPC;Apc mouse 
model. A wide-field, small animal endoscope capable of fluorescence excitation 
(450-475 nm) identified polyps via white light and also collected fluorescence 
images (510 nm barrier filter) of peptide binding. The peptide bound ~2-fold 
greater to the colonic adenomas when compared to the control. We have imaged 
fluorescence-labeled peptide binding in vivo that is specific towards distal 
colonic adenomas.
Optical-resolution photoacoustic microscopy of ischemic stroke 
Paper 7899-5 of Conference 7899
Date: Sunday, 23 January 2011
Time: 9:15 AM – 9:30 AM
Author(s): Song Hu, Konstantin Maslov, Washington Univ. in St. Louis (United 
States); Ernie Gonzales, Jin-Moo Lee, Washington Univ. School of Medicine 
(United States); Lihong V. Wang, Washington Univ. in St. Louis (United States)
Hide Abstract Add to My Schedule 
A major obstacle in understanding the mechanism of ischemic stroke is the lack 
of a tool to noninvasively or minimally invasively monitor cerebral hemodynamics 
longitudinally. Here, we applied optical-resolution photoacoustic microscopy 
(OR-PAM) to study ischemic stroke in a middle cerebral artery (MCA) occlusion 
mouse model. OR-PAM observed that within core regions of the stroke, the average 
hemoglobin oxygen saturation (sO2) within arteries/arterioles and veins drop 
~20% and ~45%, respectively, during the MCA occlusion. After reperfusion, the 
vessel sO2 in the core region recovered back to normal values. Vasodilation was 
also observed during MCA occlusion and after MCA reperfusion.
Comparison of microwave and iron-oxide nanoparticle hyperthermia 
radiosensitization in murine breast tumors 
Paper 7901-13 of Conference 7901
Date: Sunday, 23 January 2011
Time: 2:40 PM – 3:00 PM
Author(s): Andrew J. Giustini, Dartmouth Medical School (United States) and 
Dartmouth College (United States); Alicia A. Petryk, Dartmouth College (United 
States); P. Jack Hoopes, Dartmouth Medical School (United States)
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Hyperthermia is an effective radiosensitizer and has the potential to be used in 
clinical cancer therapy if it can be directed specifically to tumors. Iron oxide 
nanoparticles (IONP) excited by alternating magnetic fields have been shown to 
be an effective way to specifically heat tumors in vivo. We have demonstrated 
that the combination of IONP hyperthermia with ionizing radiation delays the 
growth of mouse breast tumors by more than double the delay achieved by either 
modality alone. We have also compared this combined IONP / radiation therapy to 
the combination of ionization radiation with microwave-induced hyperthermia.
Integrated photoacoustic and fluorescence confocal microscopy 
Paper 7899-21 of Conference 7899
Date: Sunday, 23 January 2011
Time: 3:45 PM – 4:00 PM
Author(s): Yu Wang, Konstantin Maslov, Chulhong Kim, Song Hu, Lihong V. Wang, 
Washington Univ. in St. Louis (United States)
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Optical-resolution photoacoustic microscopy has demonstrated utility in imaging 
and characterizing microvasculature networks in vivo. This work presents a novel 
imaging system that integrates optical-resolution photoacoustic microscopy and 
fluorescence confocal microscopy for simultaneous photoacoustic and fluorescence 
imaging. The integrated system can acquire intrinsically registered 
photoacoustic and fluorescence images in a single scan. The micrometer 
resolution allows imaging of blood vessels down to the capillary level. Capable 
of providing microscopic imaging of both optical absorption and fluorescence 
contrasts, the system demonstrates in vivo imaging of oxygen saturation and 
oxygen partial pressure in mouse ears.
Development of a real-time photoacoustic microscope 
Paper 7899-26 of Conference 7899
Date: Sunday, 23 January 2011
Time: 5:00 PM – 5:15 PM
Author(s): Lidai Wang, Junjie Yao, Li Li, Konstantin Maslov, Lihong V. Wang, 
Washington Univ. in St. Louis (United States)
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We present the development of a photoacoustic imaging system which has real-time 
imaging capability with optical resolution. The imaging system is capable of 
acquiring up to 40 photoacoustic frames per second depending on scanning range. 
Focused laser beams provide a lateral resolution of less than five microns. To 
demonstrate real-time imaging and high resolution, micron-sized carbon particle 
flow, whole blood flow in silicone tubing, and single red blood cell flow in a 
capillary vessel in a mouse ear were imaged in real time, which demonstrated the 
capability to image dynamic processes in vivo.
All fiber, 1064-nm time-lens source for coherent anti-Stokes Raman scattering 
and stimulated Raman scattering microscopy 
Paper 7903-29 of Conference 7903
Date: Monday, 24 January 2011
Time: 10:41 AM – 11:01 AM
Author(s): Ke Wang, Cornell Univ. (United States); Christian W. Freudiger, Brian 
G. Saar, Harvard Univ. (United States); Jennifer Lee, Cornell Univ. (United 
States); Sunney X. Xie, Harvard Univ. (United States); Chris Xu, Cornell Univ. 
(United States)
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We use the time-lens concept to demonstrate a new scheme for synchronization of 
two pulsed light sources for biological imaging. An all fiber, 1064 nm time-lens 
source is synchronized to a picosecond solid-state Ti: Saphire mode-locked laser 
by using the mode-locked laser pulses as the clock. We demonstrate the 
application of this synchronized source for CARS and SRS imaging by imaging 
mouse tissues. Synchronized two wavelength pulsed source is a major technical 
difficulty for CARS and SRS imaging. The time-lens source demonstrated here may 
provide an all fiber, user friendly alternative for future SRS imaging.
Developing targeted fluorescent contrast agents for in-vivo micropathology 
guided resection of medulloblastoma 
Paper 7910-12 of Conference 7910
Date: Monday, 24 January 2011
Time: 2:10 PM – 2:30 PM
Author(s): Danni Wang, Stony Brook Univ. (United States); Frank V. Cochran, 
Henry Haeberle, Christopher H. Contag, Stanford Univ. School of Medicine (United 
States); Jonathan T. C. Liu, Stanford Univ. (United States)
Hide Abstract Add to My Schedule 
The outcomes of brain tumor patients correlate with the degree of surgical 
resection. However, cautious resection is necessary to avoid neurological 
damage, especially in pediatric patients. Real-time image guidance will allow 
for improved resection in a larger proportion of patients, while reducing the 
debilitating effects of over-aggressive resections. We are developing in vivo 
microscopes and targeted contrast agents for guiding brain tumor resection. With 
the aid of a mouse model that spontaneously develops medulloblastoma, we are 
validating the use of both a monoclonal antibody as well as targeted 
bacteriophage as fluorescent contrast agents for the specific delineation of 
brain tumor margins in conjunction with real-time in vivo micropathology.
Silver nanoplates for enhanced photo-acoustic imaging and therapy of pancreatic 
cancer 
Paper 7910-20 of Conference 7910
Date: Monday, 24 January 2011
Time: 5:00 PM – 5:20 PM
Author(s): Kimberly A. Homan, Michael Souza, Ryan Truby, Yun-Sheng Chen, 
Geoffrey P. Luke, Stanislav Y. Emelianov, The Univ. of Texas at Austin (United 
States)
Hide Abstract Add to My Schedule 
Approaches to cancer treatment are multipronged where several methods are 
employed simultaneously to eradicate all of the cancerous tissue. Silver 
nanoplates can aid in this multiplexed approach by carrying chemotherapeutic 
drugs, targeting cancer cells, and acting as photothermal agents for cancer. 
Additionally, the large absorption cross section of the nanoplates makes them 
excellent photoacoustic imaging contrast agents. Their ability to enhance 
photoacoustic imaging in vivo in a mouse model of pancreatic cancer was 
demonstrated. Overall, silver nanoplates represent a largely unexplored 
nanosystem for cancer imaging and treatment and we demonstrate their potential 
for multifunctional imaging and treatment of pancreatic cancer.
Blind spectral unmixing identifies the molecular signatures of absorbers in 
multispectral optoacoustic tomography 
Paper 7899-123 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Nikolaos C. Deliolanis, Juergen Glatz, Andreas Buehler, Daniel 
Razansky, Vasilis Ntziachristos, Helmholtz Zentrum München GmbH (Germany)
Hide Abstract Add to My Schedule 
Deep tissue molecular imaging of contrast agents at realistic concentrations 
with photoacoustic (or optoacoustic) tomography remains a challenge. Detection 
of optical absorption contrast agents (nanoparticles, fluorochromes etc.) has 
been demonstrated by utilizing multispectral measurements, however spectral 
unmixing heavily depends on the accurate knowledge of the spectral profile of 
the absorbers. It becomes more challenging when considering that reconstruction 
algorithms might not be quantitative and also that the spectral absorption 
profile is convolved with the unknown illumination spectrum. We propose a blind 
spectral unmixing method that recovers both the spatial distribution of the 
contrast agents and their absorption spectrum and demonstrate it in whole body 
mouse imaging.
Development of a stigmatic imaging mass spectrometer using laser 
desorption/ionization 
Paper 7902-74 of Conference 7902
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Kunio Awazu, Osaka Univ. (Japan) and Univ. of Fukui (Japan) and Japan 
Science and Technology Agency (Japan); Hisanao Hazama, Hirofumi Nagao, Hidetoshi 
Yoshimura, Jun Aoki, Osaka Univ. (Japan) and Japan Science and Technology Agency 
(Japan); Kenichi Fujii, Osaka Institute of Technology (Japan) and Japan Science 
and Technology Agency (Japan); Toshio Tashima, Japan Science and Technology 
Agency (Japan); Katsuyoshi Masuda, Suntory Institute for Bioorganic Research 
(Japan) and Japan Science and Technology Agency (Japan); Michisato Toyoda, Osaka 
Univ. (Japan) and Japan Science and Technology Agency (Japan); Yasuhide Naito, 
Graduate School for the Creation of New Photonics Industries (Japan) and Japan 
Science and Technology Agency (Japan)
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We are developing a stigmatic imaging mass spectrometer which consists of a 
laser desorption/ionization ion source and a multi-turn time-of-flight mass 
spectrometer (MULTUM-IMG) for measuring multiple biomolecules simultaneously 
with a high spatial resolution and short measurement time. As the result, ion 
images were obtained with spatial resolution of 3-4 um and maintained after ten 
circulations in the multi-turn circuit of MULTUM-IMG. Ion images of dyes from a 
stained mouse brain section were successfully obtained. The measurement time 
required for observing whole part of a hippocampus was 13 minutes and reduced to 
less than 1/10 of conventional imaging mass spectrometry.
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Effect of low-power laser irradiation on macrophage phagocytic capacity 
Paper 7900-16 of Conference 7900
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Wei Chen, Feifan Zhou, Da Xing, Sheng Song, South China Normal Univ. 
(China); Wei R. Chen, Univ. of Central Oklahoma (United States) and South China 
Normal Univ. (China)
Hide Abstract Add to My Schedule 
Phagocytosis plays a pivotal role in host innate immunity. Low-power laser 
irradiation (LPLI) has been found to produce photobiological effects with 
evidence of interference with immunological functions. The effects of LPLI on 
the immune response have not been extensively characterized. In this study, we 
focused our attention on the effects of LPLI on the phagocytic activity of 
macrophages by using flow cytometry (FCM). The results showed that LPLI led to 
an increase in phagocytosis on both mouse peritoneal macrophages and the murine 
macrophage-like cell line RAW264.7.Our results indicated that LPLI with 
appropriate dosage can enhance the phagocytosis of macrophage
Longitudinal optical-resolution photoacoustic microscopy of tumor 
neovascularization 
Paper 7899-104 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Song Hu, Rebecca Sohn, Andrea C. Santeford, Konstantin Maslov, 
Jeffrey M. Arbeit, Lihong V. Wang, Washington Univ. in St. Louis (United States)
Hide Abstract Add to My Schedule 
Neovascularization is essential for tumor growth and metastasis; however, 
existing technologies have difficulty in label-free chronic imaging of tumor 
microvascular elaboration. We applied longitudinal optical-resolution 
photoacoustic microscopy (OR-PAM) for noninvasive determination of vascular 
elaboration and microcirculatory dynamics of different human cancer xenografts 
grown in mouse ears. OR-PAM determined changes in functional neovascularization 
during tumor growth and VEGF signaling inhibition. Ex-vivo tissue analysis 
co-registered tumor biological responses (tumor cell perfusion, proliferation, 
apoptosis, microvessel density, and hypoxia) with regional functional 
neovascular data acquired by OR-PAM. Combinatorial biological and OR-PAM 
analysis will facilitate novel drug design and scheduling for more effective 
antineoplastic therapies.
PER-PACT system for simultaneous imaging of acoustic properties with 
photoacoustic imaging of tumors in small animals 
Paper 7899-130 of Conference 7899
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Jithin Jose, Rene G. Willemink, Johan C. G. van Hespen, Univ. Twente 
(Netherlands); Johan W. Van Neck, Timo L. M. Ten Hagen, Univ. Medisch Ctr. 
Rotterdam, Erasmus MC (Netherlands); Wiendelt Steenbergen, Univ. Twente 
(Netherlands); Ton G. van Leeuwen, Univ. Twente (Netherlands) and Univ. van 
Amsterdam (Netherlands); Srirang Manohar, Univ. Twente (Netherlands)
Hide Abstract Add to My Schedule 
we present a system which allows simultaneous imaging of optical absorption 
properties and acoustic transmission properties of an object in a 
two-dimensional slice using a carefully positioned 'Passive' element in a 
photoacoustic imager. The passive element is placed at the far-end of the sample 
and it acts as an ultrasound source. The generated ultrasound interacts with the 
sample and can be measured using the same ultrasound detector as used for 
photoacoustic measurements.We will present detailed description of our system, 
effect of spatial distribution of SOS in photoacoustic imaging, followed by an 
iterative reconstruction algorithm which compensates for the SOS inhomogeneities 
in the imaging area. We have validated the method using appropriate phantoms and 
on a living mouse which has tumor implanted on the lower abdomen. The obtained 
images are quantitative in terms of the shape, size, location, and acoustic 
properties of the examined heterogeneities.
Multi-target photoacoustic molecular imaging of cardiovascular inflammatory 
biomarkers using bioconjugated gold nanorods 
Paper 7899-57 of Conference 7899
Date: Tuesday, 25 January 2011
Time: 8:15 AM – 8:30 AM
Author(s): Seunghan Ha, Sakya Tripathy, Linda L. Lavery, Andrew Carson, Univ. of 
Pittsburgh Medical Ctr. (United States) and Univ. of Pittsburgh (United States); 
Ashish Agarwal, Nicholas A. Kotov, Univ. of Michigan (United States); Flordeliza 
S. Villanueva, Kang Kim, Univ. of Pittsburgh Medical Ctr. (United States) and 
Univ. of Pittsburgh (United States)
Hide Abstract Add to My Schedule 
Multiple cardiovascular inflammatory biomarkers were simultaneously imaged in 
vivo. A mouse model based on the vascular endothelium injury by a photochemical 
reaction of Rose Bengal dye to green light was used. Goldnanorods (GNR) (800nm) 
conjugated to ICAM-1 antibody and E-selectin antibody conjugated GNR (715nm) 
were injected. Photoacoustic intensity measured by a commercial ultrasound probe 
synchronized to a pulsed laser (10mJ/cm^2) at 715nm or 800nm clearly identified 
the upregulations of targeted biomarkers. Histopathology of the harvested 
tissues confirmed inflammation. The feasibility of simultaneous targeting and 
monitoring of inflammation responses in cardiovascular system using a commercial 
ultrasound has been demonstrated in vivo.
In vivo photoacoustic detection, magnetic enrichment and photothermal purging of 
circulating cancer stem cells targeted by nanoparticles 
Paper 7899-58 of Conference 7899
Date: Tuesday, 25 January 2011
Time: 8:30 AM – 8:45 AM
Author(s): Ekaterina I. Galanzha, Univ. of Arkansas for Medical Sciences (United 
States); Jin-Woo Kim, Univ. of Arkansas (United States); Lyuba Varticovski M.D., 
National Cancer Institute (United States)
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Circulating cancer stem cells represent a rare, therapy-resistant subset of 
circulating tumor cells (CTCs) that hypothetically initiate metastasis. This 
study pioneered clinically-relevant multicolor high-speed photoacoustic flow 
cytometry for in vivo detection, enrichment, and eradication of cancer stem 
cells in peripheral blood circulation. As demonstrated in a breast-tumor-bearing 
mouse model, our platform is capable real-time enumeration and molecular 
characterization of circulating cancer stem cells during tumor progression with 
an unprecedented sensitivity threshold at one tumor cell among a billion normal 
blood cells. These preclinical studies may provide a new, advanced theranostic 
strategy to improve early diagnosis and therapy of metastatic tumors.
Ultra-high-resolution and ultra-high-sensitive optical micro-angiography based 
on supercontinuum light source 
Paper 7889-40 of Conference 7889
Date: Tuesday, 25 January 2011
Time: 11:45 AM – 12:00 PM
Author(s): Zhongwei Zhi, Lin An, Jia Qin, Ruikang K. Wang, Oregon Health & 
Science Univ. (United States)
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We demonstrate for the first time an ultrahigh resolution and ultrahigh 
sensitive optical micro-angiography (UHS-OMAG) system that is realized by a 
supercontinuum light source and an ultrafast CMOS camera. The broad band light 
source with a central wavelength at ~800nm, emitted from the supercontinuum 
light source, provides a ~2µm coherence gate for the system. With the fast CMOS 
camera employed in the spectrometer operating at ~70 kHz line rate, we 
demonstrate that the detailed blood vessel networks, including capillaries, 
buried within the tissue bed can be visualized. We present the results obtained 
from the human finger nail fold and the mouse ear flap. The excellent system 
imaging performance shows a great potential of our system in the future 
biological imaging application.
Multimodal optical coherence/photo-acoustic tomography of skin 
Paper 7889-41 of Conference 7889
Date: Tuesday, 25 January 2011
Time: 1:30 PM – 1:45 PM
Author(s): Aneesh P. Alex, Cardiff Univ. (United Kingdom); Edward Z. Zhang, 
Univ. College London (United Kingdom); Boris Považay, Medizinische Univ. Wien 
(Austria); Jan G. Laufer, Univ. College London (United Kingdom); Bernd Hofer, 
Medizinische Univ. Wien (Austria); Carl Glittenberg M.D., Ludwig Boltzmann 
Institut (Austria); Boris Hermann, Medizinische Univ. Wien (Austria); Paul C. 
Beard, Univ. College London (United Kingdom); Wolfgang Drexler, Medizinische 
Univ. Wien (Austria)
Hide Abstract Add to My Schedule 
A novel non-invasive in vivo multimodal optical coherence tomography 
(OCT)/photoacoustic tomography (PAT) imaging system capable of obtaining 
structural and functional information simultaneously has been demonstrated in 
skin. A 1060 nm OCT system acquiring 47k depth-scans/s with ~7 µm axial and ~ 20 
µm transverse resolutions has been incorporated into a backward-mode PA system. 
For PAT, the excitation wavelength was set to 670 nm and a focused laser beam at 
1550 nm was used as the sensor interrogation beam. OCT and PAT images were 
obtained sequentially from a hairless mouse and the co-registered images were 
combined to form the final 3D image.
Diagnosing lung cancer using coherent anti-Stokes Raman scattering microscopy
Paper 7890-41 of Conference 7890
Date: Tuesday, 25 January 2011
Time: 3:30 PM – 3:50 PM
Author(s): Liang Gao, Rice Univ. (United States) and Methodist Hospital Research 
Institute (United States); Fuhai Li, Jiong Xing, Methodist Hospital Research 
Institute (United States); Michael J. Thrall, The Methodist Hospital (United 
States); Yaliang Yang, Zhiyong Wang, Pengfei Luo, Methodist Hospital Research 
Institute (United States); Kelvin K. Wong, Methodist Hospital Research Institute 
(United States) and The Methodist Hospital (United States); Hong Zhao, Methodist 
Hospital Research Institute (United States); Stephen T. C. Wong, Methodist 
Hospital Research Institute (United States) and The Methodist Hospital (United 
States) and Rice Univ. (United States)
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Lung carcinoma is the most prevalent type of cancer in the world, and it is 
responsible for more deaths than other types of cancer. Early detection of lung 
cancer can dramatically increase the survival rate. We investigated the 
feasibility of developing coherent anti-Stokes Raman scattering (CARS) 
microscopy into an early detection strategy for lung cancer using mouse models. 
CARS images from normal lung tissues and different subtypes of cancer lesions 
showed good correlation with their corresponding histological staining with 
regard to pathologically prevalent features, supporting the idea of applying 
CARS in vivo for label-free and minimally-invasive differential diagnostic 
applications.
Multiphoton fluorescence lifetime imaging of cleared tissue 
Paper 7903-84 of Conference 7903
Date: Tuesday, 25 January 2011
Time: 5:50 PM – 6:05 PM
Author(s): Michael J. Levene, Sam Vesuna, Sonia Parra, Thomas H. Chia, Yale 
Univ. (United States)
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Optical clearing of fixed tissue enables multiphoton microscopy (MPM) of 
intrinsic fluorescence to depths of >2 mm in tissue. Large MPM image stacks of 
BABB cleared tissue offer great opportunity for advancing optical biopsy 
techniques and 3D histology through the development of 'virtual organs' that are 
compatible with traditional histological sample preparations, potentially easing 
its acceptance by the medical community. However, intrinsic sources of 
fluorescence in tissues often display broad excitation and emission spectra, 
complicating the ability to achieve molecular contrast. We present MPM-FLIM 
images of intrinsic fluorescence from mouse organs and human prostate biopsy 
samples cleared with BABB.
Two-photon fluorescence vascular imaging with a new fluorene-RGD peptide 
conjugate 
Paper 7910-41 of Conference 7910
Date: Wednesday, 26 January 2011
Time: 8:20 AM – 8:40 AM
Author(s): Kevin D. Belfield, Alma R. Morales, Univ. of Central Florida (United 
States); Takeo Urakami, Junko Sawada, Sanford-Burnham Medical Research Institute 
(United States); Ciceron O. Yanez, Univ. of Central Florida (United States); 
Masanobu Komatsu, Sanford-Burnham Medical Research Institute (United States)
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Multiphoton fluorescence microscopy is a powerful tool in the study of living 
cells, and features of microvasculature. In the present study, a 2PFM 
interactive image-analysis method was utilized to evaluate the efficiency of a 
new 2PA conjugate which was designed to target avß3 integrin. The linear and 
nonlinear photophysical properties of this RGD peptide fluorescent conjugate 
were carefully measured. This conjugate was injected into the tail vein of a 
male C5BL/6 mouse that had been implanted subcutaneously with Lewis Lung 
Carcinoma cells. The excised tumors consisting of ~ 1 cm3 in volume were 
whole-mounted and imaged by 2PFM. Ex vivo 2PFM revealed the structure of 
functional vessels deep within the tumor mass.
Refractive index reconstruction of biological samples from multimodal phase 
microscopy 
Paper 7904-25 of Conference 7904
Date: Wednesday, 26 January 2011
Time: 9:40 AM – 10:00 AM
Author(s): Heidy Sierra, Dana H. Brooks, Charles A. DiMarzio, Northeastern Univ. 
(United States)
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Extraction of quantitative information is important to better understand 
cellular activity in biological preparations. In particular the optical 
refractive index can be used to analyze the results of cellular processes. Phase 
microscopy modalities are widely used to image unstained biological samples. 
Here we present a constrained boundary iterative method to reconstruct the 
spatial distribution of refractive index combining information from two phase 
microscopy techniques. Simulations have confirmed the reliability of the 
proposed method. Experiments with measurements from mouse embryos at several 
development stages show that the proposed approach can reconstruct the 
distribution of the refractive index of these samples.
Dynamic in-vivo visualization of anastomosis between a prevascularized 
implantable tissue construct and host circulation 
Paper 7897-50 of Conference 7897
Date: Wednesday, 26 January 2011
Time: 11:20 AM – 11:40 AM
Author(s): Sean White, Christopher Hughes, Bernard Choi, Steven C. George M.D., 
Univ. of California, Irvine (United States)
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The thickness of implantable engineered tissue is restricted by the relatively 
short diffusion path length of oxygen. One method for overcoming this 
limitation, termed prevascularization, entails the in vitro formation a vascular 
network within an engineered tissue construct capable of anastomosing with the 
host circulation following implantation. We utilized mouse dorsal window 
chambers to facilitate dynamic imaging of prevascularized tissue implants using 
laser speckle imaging, multispectral imaging, and multiphoton microscopy. This 
permits in vivo dynamic visualization and quantification of anastomosis and 
implant perfusion, and may be used to enhance the design of thick tissue 
engineered constructs and mechanisms of anastomosis.
Aberration correction in harmonic generation microscopy 
Paper 7931-16 of Conference 7931
Date: Thursday, 27 January 2011
Time: 2:45 PM – 3:10 PM
Author(s): Alexander Jesacher, Innsbruck Medical Univ. (Austria); Anisha Thayil, 
Tomoko Watanabe, Tony Wilson, Shankar Srinivas, Martin J. Booth, Univ. of Oxford 
(United Kingdom)
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In harmonic generation microscopy, the sample is scanned with a focused 
short-pulsed laser beam and the second and/or third harmonic signal which is 
generated by the specimen is collected. Although the wavelength of the scanning 
beam can be in the near infrared, which implies a large penetration depth and 
low scattering, aberrations introduced by imperfect optics and specimen 
inhomogenity can have a large effect on image brightness, contrast and 
resolution. We show how aberrations in a harmonic generation microscope can be 
measured and corrected using modal wavefront sensing and a deformable mirror, 
which is integrated into the optical path of the microscope. We present results 
obtained from short- and long-term imaging of live mouse embryos.
Adaptive optics two photon scanning laser fluorescence microscopy 
Paper 7931-17 of Conference 7931
Date: Thursday, 27 January 2011
Time: 3:40 PM – 4:05 PM
Author(s): Yaopeng Zhou, GE Healthcare (United States); Thomas Bifano, Boston 
Univ. (United States); Charles Lin, Wellman Ctr. for Photomedicine (United 
States)
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Two-photon scanning laser fluorescence microscopy provides a powerful tool for 
deep tissue imaging. However, optical aberrations from illumination beam path 
limit the peak power delivered to the imaging planes at samples. We have 
developed an AO system relying on a MEMS Deformable Mirror to compensate the 
optical aberrations in a two-photon scanning laser fluorescence microscope. The 
AO system utilized a Zernike polynomial based stochastic parallel gradient 
descent algorithm to optimize the DM shape for wavefront correction. The 
developed microscope is applied for subsurface imaging of mouse bone marrow.
Adaptive optics confocal fluorescence microscopy with direct wavefront sensing 
for brain tissue imaging 
Paper 7931-21 of Conference 7931
Date: Thursday, 27 January 2011
Time: 5:10 PM – 5:25 PM
Author(s): Xiaodong Tao, Bautista R. Fernandez, Univ. of California, Santa Cruz 
(United States); Diana C. Chen, Lawrence Livermore National Lab. (United 
States); Oscar A. Azucena, Min Fu, Yi Zuo, Joel Kubby, Univ. of California, 
Santa Cruz (United States)
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Recently, there has been a growing interest in deep tissue imaging for the study 
of neurons. Unfortunately, because of the inhomogeneous refractive index of the 
tissue, the aberrations degrades the resolution and brightness of the final 
image. In this paper, we describe a confocal fluorescence microscope with 
adaptive optics which can correct aberrations based on direct wavefront 
measurements using a point source reference beacon and a Shack-Hartmann 
Wavefront Sensor (SHWS). The mouse brain tissues with different thicknesses are 
tested. After correction, the near diffraction limited image is achieved. The 
Strehl ratio increased by 70% after correction for the tissue with the thickness 
of 100µm.
Non-invasive in-vivo micro-Raman spectroscopy of a murine skin tumor model 
reveals cancer-specific spectral biomarkers 
Paper 7883A-4 of Conference 7883A
Date: Saturday, 22 January 2011
Time: 9:00 AM – 9:20 AM
Author(s): Hequn Wang, Naiyan Huang, Jianhua Zhao, The BC Cancer Agency Research 
Ctr. (Canada); Harvey Lui M.D., The Univ. of British Columbia (Canada); Mladen 
Korbelik, Haishan Zeng, The BC Cancer Agency Research Ctr. (Canada)
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We developed a micro-Raman spectrometer system for differentiating tumor lesions 
from normal skin using an in vivo animal model. A study of 494 Raman spectra 
from 24 mice revealed different spectral patterns at different depths and 
between normal and tumor bearing skin sites. A peak at 899 cm-1 (possibly from 
proline or fatty acids) and one with higher intensity in the 1325 - 1330 cm-1 
range (assigned to nucleic acids) were correlated with the presence of tumors 
and could potentially be used as biomarkers for skin cancer detection. Spectral 
diagnosis achieved diagnostic sensitivity of 95.8% and specificity of 93.8%.
Evaluation of the use of antibody conjugated plasmonic nanoparticles for brain 
tumor delineation 
Paper 7883E-100 of Conference 7883E
Date: Saturday, 22 January 2011
Time: 10:40 AM – 11:00 AM
Author(s): Kevin C. Seekell, Christy Wilson, Gerald Grant, Adam P. Wax, Duke 
Univ. (United States)
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Complete resection of a pediatric brain tumor is a major factor in the survival 
rates of patients following surgery. Therefore, delineation of the brain tumor 
is an essential tool in helping the surgeon to remove the entire tumor while 
retaining normal tissues. In this study, the use of immunolabled plasmonic gold 
nanoparticles as intraoperative contrast agents for tumor delineation was 
tested. A modified microscope was designed to separately image bioluminescence 
and nanorod scattering from brain slices of nude mice. Both delineation methods 
identified the same areas on the samples with high specificity. Immunolabeled 
gold nanoparticles are effective for tumor delineation.
Size and surface chemistry of Au nanoparticles determine doxorubicin 
cytotoxicity 
Paper 7909-51 of Conference 7909
Date: Saturday, 22 January 2011
Time: 11:20 AM – 11:40 AM
Author(s): Jay L. Nadeau, Hicham Chibli, Xuan Zhang, McGill Univ. (Canada)
Hide Abstract Add to My Schedule 
Several formulations of gold-doxorubicin conjugates (Au-Dox) have been reported. 
However, the effects of particle size, lability of the conjugating bond, and 
specific targeting have not been fully explored. In this work we compare the 
relative cytotoxicity of 5 nm vs. 2 nm Au-Dox, and explore the effects of 
polyethylene glycol (PEG) and specific cell-targeting sequences on toxicity in 
B16 melanoma cells and in mice. We find that Au-Dox does not show increased 
cytotoxicity over Dox alone unless the particles are small enough to enter the 
nucleus. Surprisingly, cleavable bonds do not increase effectiveness, with even 
stably-bonded Au-Dox showing maximum cytotoxicity in less than one hour. 
Preliminary studies on molecular mechanisms of action implicate reactive oxygen 
species formation leading to apoptosis as the primary cause of cell destruction, 
with Dox-resistant cancer cells showing reduced resistance to Au-Dox. These 
results have important implications for the development of Au nanoparticle-based 
anticancer agents.
Photobiomodulatory effects of He-Ne laser on excision wounds 
Paper 7887-16 of Conference 7887
Date: Saturday, 22 January 2011
Time: 4:00 PM – 4:20 PM
Author(s): Vijendra Prabhu, Satish B. S. Rao, Manipal Univ. (India); Pramod 
Kumar, ; Lakshmi Rao, Manipal University (India); Krishna K. Mahato, Manipal 
Univ. (India)
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The present study was aimed to investigate the promotive effect of LLLT on 
excision wounds in Swiss albino mice using optical fiber probe based light 
device. Excision wounds were illuminated with single exposure of various laser 
doses except controls. Further, optimal dose of 2 J/cm2 was applied to excision 
wounds at different post-wounding treatment schedules. Progression of wound 
contraction, mean wound healing time and biochemical estimations from wound 
ground tissue were assessed. Granulation tissues were stained with 
Hematoxylin-Eosin staining and analyzed. Results demonstrated optimum tissue 
regeneration at 2 J/cm2 dose, applied immediately after the wounding as compared 
to controls.
Dual-drug MRI-FMT for quantification of binding affinity in vivo 
Paper 7892-21 of Conference 7892
Date: Saturday, 22 January 2011
Time: 5:40 PM – 6:00 PM
Author(s): Scott C. Davis, Kimberley S. Samkoe, Julia A. O'hara, Kristian J. 
Sexton, Keith D. Paulsen, Brian W. Pogue, Dartmouth College (United States)
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This study examines specific binding of a receptor-targeted imaging agent in 
brain tumors using simultaneous MR-guided fluorescence molecular tomography 
(FMT) of two optical probes. Glioma cells which over-express epidermal growth 
factor receptor (EGFR) were grown in the brains of nude mice. Imaging began with 
the co-injection of two NIR fluorescence probes with different emission spectra; 
one probe targeted to EGFR and the other a negative control. Animals were imaged 
using an MRI-FMT system with spectrometer-based detectors. Spectrally unmixed 
signals were used to recover images of fluorescence yield of both drugs, 
facilitating the quantification of specific binding of the EGFR-targeted probe.
Modelling and characterization of photothermal effects assisted with gold 
nanorods in ex-vivo samples and in a murine model 
Paper 7901-12 of Conference 7901
Date: Sunday, 23 January 2011
Time: 2:20 PM – 2:40 PM
Author(s): Felix Rodriguez, Sr., Horacio Rivera Lamela, Sr., Vincent B. 
Cunningham, Univ. Carlos III de Madrid (Spain)
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We discuss in this article the implementation of a laser-tissue interaction and 
bioheat-transfer 2-D finite-element model for Photothermal Therapy (PTT) 
assisted with Gold Nanorods. We have selected Gold Nanorods as absorbing 
nanostructures in order to improve the efficiency of using compact diode lasers 
because of their high opto-thermal conversion efficiency at NIR spectra. The 
goal is to model the distribution of the optical energy among the tissue 
including the skin absorption effects and the tissue thermal response, with and 
without the presence of Nanorods. The heat generation due to the optical energy 
absorption and the thermal propagation will be computationally modeled and 
optimized. The model has been evaluated and compared with experimental ex-vivo 
data in fresh chicken muscle samples and in-vivo murine model. Finally, we will 
study the PTT in tumors by using the CT-26 human cancer cell-line to induce the 
corresponding xenografts in the animal's back of these BALB/c mice.
How does temperature affect the function of tissue macrophages? 
Paper 7901-16 of Conference 7901
Date: Sunday, 23 January 2011
Time: 4:30 PM – 4:45 PM
Author(s): Chen-Ting Lee, Roswell Park Cancer Institute (United States)
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Macrophages sound a danger signal following injury or infection and become 
activated to release pro-inflammatory cytokines. Usually, tissue macrophages are 
exposed to an elevated temperature during inflammation. However, whether 
macrophages respond to temperature change to modulate their function is not 
clear. Here we studied thermal effects on macrophage functions from 
LPS-challenged mice at early or late activation stages which are representative 
of the initiation and resolution phases of inflammation. Our data suggest that 
in the initiation phase, thermal stress acts as a stimulus to enhance macrophage 
functions. However, for previously activated macrophages, thermal stress 
provides a negative signal that suppresses their cytokine production. These 
results increase our understanding of the role of elevated tissue temperature on 
modulation specific functions of macrophages. They also provide additional 
rationale for the use of hyperthermia in the treatment of chronic inflammation.
A hybrid approach combining microCT and fluorescence tomography: imaging 
workflow and system of coordinate registration 
Paper 7892-41 of Conference 7892
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Robert Holt, Fadi El-Ghussein, Dartmouth College (United States); 
Kenneth M. Tichauer, Lawson Health Research Institute (Canada); Frederic 
Leblond, Brian W. Pogue, Dartmouth College (United States)
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A fluorescence imaging system was designed to interface with a microCT device. 
We focus on refining the workflow for meshing and the co-registration of the two 
systems. The former is performed by projection imaging in the microCT, 
reconstructing a volume, segmenting using image processing software, and meshing 
using NIRFAST. Co-registration is performed by exploiting the geometry of the 
fluorescence system. We determine the location of the geometrical center of a 
subject, which can be used to derive a translation between instruments. The 
co-registration will be validated by imaging a synthetic mouse phantom, as well 
as actual mice with implanted fluorophore concentrations.
Combination of optical imaging with NIR fluorophore and sonogram in breast 
cancer diagnosis 
Paper 7886-45 of Conference 7886
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Kuo-Chih Liao, Tsung-Hsien Yen, Gi-Da Lee, Yu-Hsiang Chou, National 
Chung Hsing Univ. (Taiwan)
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The project will evaluate the potential of the combination imaging tools 
(optical imaging with near infrared fluorophore, SIDAG, and sonogram) for 
non-invasive, low facility requirement and low cost breast cancer diagnosis. The 
average value of optical and echo signals from normal tissue, benign lesion 
xenografts (extracellular membrane extract from the EHS mouse sarcoma) and 
malignant tumor xenografts (MCF-7 cell) developed in nude mice will be recorded 
and mapped for the following procedures: 1. Average threshold value of contrasts 
among the normal tissue, benign lesion xenograft and malignant tumor xenograft 
(screening). 2. Size and boundary of tumor tissue (staging of cancer). 3. Size 
and boundary of tumor tissue before and after chemotherapy (evaluation of 
treatment).
Evaluation of laser photobiomodulation in repair of cutaneous wounds in rats 
infected of staphylococcus aureus 
Paper 7887-32 of Conference 7887
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Nicole Ribeiro Santos, Priscila C. Oliveira, Jean Nunes dos Santos, 
Antônio L. Barbosa Pinheiro, Univ. Federal da Bahia (Brazil)
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This work has as objective evaluates through a histological study the action of 
the laser in cutaneous wounds infected by Staphylococus aureus. Sixty mice will 
be used (Wistar), being accomplished in the back of each animal a wound of 1cm2, 
the animals will be divided in four groups: group control, group laser ?680nm; 
group Laser ?790nm; group Laser ?680nm + ?790nm (7 and 14 days; 10, 20 and 
30J/cm2 . It is concluded that lasertehrapy resulted in a better repair in the 
groups with 20 e 30J/cm2 and ?680 and ?790nm laser light.
In-vivo validation of high-frequency ultrasound-guided fluorescence tomography 
system to improve delivery of photodynamic therapy 
Paper 7886-37 of Conference 7886
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Akshat Paliwal, The Cleveland Clinic (United States); Sason Torosean, 
Josiah D. Gruber, Julia A. O'Hara, Brian W. Pogue, Dartmouth College (United 
States); Tayyaba Hasan, Massachusetts General Hospital (United States); Edward 
V. Maytin, The Cleveland Clinic (United States)
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PDT for skin cancer is sometimes only partially effective, due to inadequate 
levels of the fluorescent drug (PPIX) and its heterogeneous distribution. To 
image the PPIX distribution within tissue, we developed a fluorescence 
tomography system (FTS) that combines fluorescence detection array with high 
frequency ultrasound transducer. Validation experiments were performed in vivo 
using A431 tumor-bearing mice were treated with 5-aminolevulinic acid to induce 
production of PPIX. FTS reconstructions were compared with histology and data 
from bulk tumor slices imaged using ex vivo fluorescence scanner. Our data 
demonstrate the feasibility of using the FTS for subsurface imaging of PPIX in 
vivo.
Mechanisms of tumor necrosis in photodynamic therapy with a chlorine 
photosensitizer: experimental studies 
Paper 7886-44 of Conference 7886
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Valeriy A. Privalov, Alexander V. Lappa, Elmir N. Bigbov, Chelyabinsk 
State Univ. (Russian Federation)
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A PDT experiment on 118 inbred white mice with transplanted Ehrlich's 
adenocarcinoma is performed to reveal mechanisms of necrosis formation. There 
were used a chlorine type photosensitizer "Radachlorine", and 662 nm wavelength 
diode laser. Histological investigations were conducted in different follow-up 
periods, they included optical microscopy, immune marker analysis, morphometry 
with measurements of volume density of epithelium, tumor stroma and necroses, 
vascular bed. The investigations showed that one of the main mechanisms of tumor 
necrosis development after PDT is the hypoxic damage of tumor, provided by 
disturbances of microcirculatory bed. Four stages of necrosis formation are 
specified and described in the work.
Single-particle imaging by two-photon microscopy in vivo 
Paper 7903-100 of Conference 7903
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Lisa Krapf, Univ. zu Lübeck (Germany); Jelena Dimitrijevic, Univ. 
Hamburg (Germany); Anna Schüth, Univ. zu Lübeck (Germany); Tobias Vossmeyer, 
Univ. Hamburg (Germany); Andreas Gebert, Univ. zu Lübeck (Germany); Horst 
Weller, Univ. Hamburg (Germany); Gereon Hüttmann, Univ. zu Lübeck (Germany)
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Due to the excellent penetration of NIR light in biological tissue, two-photon 
excitation laser scanning microscopy is an ideal tool to study morphology and 
dynamic processes in living tissue. Here, this technique is employed to 
investigate the interaction of nanoparticles with cells of the small intestine. 
As tracking of single nanoparticles is hampered by a mostly strong tissue 
autofluorescence, highly luminescent nanoparticles are required. We here show 
that semiconductor nanocrystals possess a sufficient cross section for 
two-photon excitation and that single nanocrystals can be detected. This 
approach was successfully used for studying in vivo particle uptake by the small 
intestinal mucosa of mice.
Transport-theory based multispectral imaging with PDE-constrained optimization
Paper 7896-91 of Conference 7896
Date: Sunday, 23 January 2011
Time: 5:30 PM
Author(s): Hyun-Keol Kim, Molly L. Flexman, Michael Khalil, Andreas H. 
Hielscher, Columbia Univ. (United States)
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We present a transport-theory-based PDE-constrained multispectral method for 
direct imaging of the spatial distributions of chromophores concentrations in 
biological tissue. The method solves the forward problem and the inverse problem 
in an all-at-once manner in the framework of a reduced Hessian sequential 
quadratic programming method. To illustrate the code's performance, we present 
numerical and experimental/clinical studies involving tumor bearing mice and 
diabetes feet. It is shown that the PDE-constrained multispectral method 
accelerates the reconstruction process by up to 15 times compared to 
unconstrained reconstruction algorithms and provides more accurate results as 
compared to the so-called two-step approach to multi-wavelength imaging.
Distribution of quantum dots after intraperitoneal administration, with 
reference to area-specific distribution in the brain 
Paper 7909-38 of Conference 7909
Date: Monday, 24 January 2011
Time: 8:30 AM – 9:00 AM
Author(s): Shinji Fushiki M.D., Kyoko Itoh M.D., Shingo Kato, Takeshi Yaoi, 
Masafumi Umekage, Takenori Tozawa, Kyoto Prefectural Univ. of Medicine (Japan); 
Yutaka Yoshikawa, Hiroyuki Yasui, Kyoto Pharmaceutical Univ. (Japan); Akiyoshi 
Hoshino, Noriyoshi Manabe, Kenji Yamamoto M.D., International Medical Ctr. of 
Japan (Japan)
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The brain is a challenging organ for drug delivery due to the presence of the 
blood brain barrier. Here, we evaluated the tissue distribution of bioconjugated 
quantum dots(QDs), i.e., captopril-conjugated QDs (QDs-cap) following 
intraperitoneal injection into mice, employing ICP-MS and confocal microscopy 
coupled with spectrometric analysis. We demonstrated that intraperitoneally 
administered QDs-cap were delivered via systemic blood circulation into visceral 
organs at 6 hours after injection. Although QDs-cap were located predominantly 
inside the blood vessels in liver, kidney and brain, but a few were distributed 
in the parenchyma, especially noteworthy in the brain.
Quantification of optical absorption coefficients from acoustic spectra with 
photoacoustic tomography 
Paper 7899-31 of Conference 7899
Date: Monday, 24 January 2011
Time: 8:45 AM – 9:00 AM
Author(s): Zijian Guo, Song Hu, Christopher P. Favazza, Washington Univ. in St. 
Louis (United States); Todd N. Erpelding, Ladislav Jankovic, Philips Research 
North America (United States); Lihong V. Wang, Washington Univ. in St. Louis 
(United States)
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Optical absorption is closely associated with many physiologically important 
parameters, such as the concentration and oxygen saturation of hemoglobin, and 
it can be used to quantify the concentrations of non-fluorescent molecules. We 
introduce a method to quantify the absolute optical absorption based upon the 
acoustic spectra of photoacoustic (PA) signals. This method has been implemented 
on various PA systems, including optical-resolution PA microscopy, 
acoustic-resolution PA microscopy, and reconstruction based PA array systems. We 
quantified the optical absorption coefficients of copper chloride samples at 
various wavelengths. We also quantified the oxygen saturation of hemoglobin in 
live mice.
Imaging the small animal cardiovascular system in real-time with multispectral 
optoacoustic tomography 
Paper 7899-38 of Conference 7899
Date: Monday, 24 January 2011
Time: 11:00 AM – 11:15 AM
Author(s): Adrian Taruttis, Eva Herzog, Daniel Razansky, Vasilis Ntziachristos, 
Helmholtz Zentrum München GmbH (Germany)
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Multispectral Optoacoustic Tomography (MSOT) is an emerging technique for high 
resolution macroscopic imaging with optical and molecular contrast. We present 
cardiovascular imaging results from a multi-element real-time MSOT system 
recently developed for studies on small animals. Anatomical features relevant to 
cardiovascular disease, such as the carotid arteries, the aorta and the heart, 
are imaged in mice. The system's fast acquisition time, in tens of microseconds, 
allows images free of motion artifacts from heartbeat and respiration. 
Additionally, we present in-vivo detection of indocyanine green and gold 
nanorods at high spatial and temporal resolution, paving the way for molecular 
imaging applications.
Study on the modulation of cellular activity through the integration of gold 
nanostructured and laser therapy 
Paper 7900-14 of Conference 7900
Date: Monday, 24 January 2011
Time: 4:50 PM – 5:10 PM
Author(s): Emiliano de Oliveira Barreto, Fabíola de Almeida Brito, Rafael V. 
Santos, Eduardo J. S. Fonseca, Jandir M. Hickmann M.D., Univ. Federal de Alagoas 
(Brazil)
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Gold nanoparticles (NPAu) have been attracting growing interest over the last 
decade because of their unique optical properties and biocompatibility for use 
in diagnosis, treatment, and as delivery vectors for biologic or pharmacologic 
agents. The low power laser irradiation (LPLI) is a non-invasive procedure that 
promotes a beneficial effect in several biological events. However, the effects 
of LPLI on cells exposed to gold nanoparticle (NPAu) are poorly understood. This 
study was undertaken to evaluate the effects of LPLI on proliferative response 
of the cells loaded with gold nanoparticles in vitro. For this, lymphocytes 
isolated of the lymph from naive mice were incubated overnight with NPAu and 
exposed to LPLI (10 mW) with variable treatment time. After 4 h the cell 
morphology and viability were evaluated by optical microscopy and MTT assay, 
respectively. We will present these evaluations for the lymphocytes incubated 
with and without (control group) NPAu.
Sensing and enumerating rare circulating cells with diffuse light 
Paper 7902-79 of Conference 7902
Date: Monday, 24 January 2011
Time: 5:30 PM
Author(s): Eric W. Zettergren, Mark J. Niedre, Northeastern Univ. (United 
States)
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The goal of this research is to develop a method for enumerating rare 
circulating cells in-vivo with diffuse light allowing interrogation of larger 
blood vessels and blood volumes than currently possible. Our initial instrument 
is capable of detecting and counting single, calibrated cell-simulating 
fluorescent mircospheres when passed through a limb-mimicking flow phantom with 
similar optical properties, size and flow rates as the limb of a mouse. 
Characterization with Vybrant-DiD labeled cells was also performed. Future work 
includes testing of the instrument using circulating, fluorescently labeled 
T-Lymphocyte cells in mice in-vivo.
Gold nanoparticles for theranostic 
Paper 7910-23 of Conference 7910
Date: Tuesday, 25 January 2011
Time: 8:30 AM – 8:50 AM
Author(s): Marina A. Sirotkina, Vadim V. Elagin, Marina V. Shirmanova, Nizhny 
Novgorod State Medical Academy (Russian Federation); Pavel D. Agrba, Institute 
of Applied Physics (Russian Federation); Victor A. Nadtochenko, N.N. Semenov 
Institute of Chemical Physics (Russian Federation); Elena V. Zagaynova, Nizhny 
Novgorod State Medical Academy (Russian Federation)
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In the present study we used bifunctional gold nanoparticles which are optimal 
for optical coherence tomography (OCT) diagnostics and laser heating. Gold 
nanoparticles were injected intravenously. The study was performed on CBA mice 
bearing cervical carcinoma. Noninvasive control of nanoparticle accumulation in 
tumor was carried out by the OCT device. Laser treatment was performed in 5 
hours after nanoparticle injection. The tumor temperature was controlled to be 
45°C. Histopathology and electron microscopy studies were conducted to observe 
the cell death in tumor. The anti-tumor impact of hyperthermia is confirmed by 
inhibition of tumor growth and induced apoptotic death of tumor cells.
Label-free 3D optical imaging of microcirculation within sentinel lymph node in 
vivo 
Paper 7889-35 of Conference 7889
Date: Tuesday, 25 January 2011
Time: 10:30 AM – 10:45 AM
Author(s): Yeongri Jung, Zhongwei Zhi, Ruikang K. Wang, Oregon Health & Science 
Univ. (United States)
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Sentinel lymph node (SLN) is the first lymph node to drain wastes originated 
from cancerous tissue. There is a need for an in vivo imaging method that can 
image the intact SLN in order to further our understanding of its normal as well 
as abnormal functions. We report the use of ultrahigh sensitive optical 
microangiography (UHS-OMAG) to image functional microvascular and lymphatic 
vessel networks that innervate the intact lymph node in mice in vivo. The 
promising results show a potential role of UHS-OMAG in the future understanding 
and diagnosis of the SLN involvement in cancer development.
Imaging tumor specific peptide-targeting using spectral-domain optical coherence 
tomography 
Paper 7890-31 of Conference 7890
Date: Tuesday, 25 January 2011
Time: 11:10 AM – 11:30 AM
Author(s): Ping Yu, Lixin Ma, Univ. of Missouri-Columbia (United States)
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We report imaging studies on tumor specific peptide-targeting in mice using a 
newly developed spectral-domain optical coherence tomography (SD-OCT). The 
system used two central wavelengths and an electro-optic modulation in the 
reference is used to get full-range deep imaging inside tumor. The optical 
probes were based on Bombesin (BBN). The SD-OCT imaging can identify normal 
tissue and tumor tissue through the difference in scattering coefficient, and 
trace the BBN probes in a severely compromised immunodeficient mouse model 
bearing human PC-3 prostate tumor xenografts. Our results demonstrated that 
SD-OCT is a potential tool for pre-clinical and clinical early cancer detection.
Application of near-infrared fluorescence imaging to monitor changes in HER2 
expression after therapeutic intervention 
Paper 7910-35 of Conference 7910
Date: Tuesday, 25 January 2011
Time: 5:00 PM – 5:20 PM
Author(s): Victor V. Chernomordik, Moinuddin Hassan, Rafal Zielinski, Amir H. 
Gandjbakhche, Jacek Capala, National Institutes of Health (United States)
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A method to quantify the overexpression of HER2 receptor in the tumor is 
suggested. Quantitative in vivo NIR optical imaging of xenografts mice with 
subcutaneous HER2-positive tumors was performed. Fluorescence images were 
obtained at several time points after intravenous injection of the dye to 
investigate binding kinetics. Compartmental ligands-receptor model was used to 
estimate HER2 expression from data, obtained with HER2-specific contrast agent, 
and monitor treatment with 17-DMAG. Initial slope, characterizing the temporal 
dependence of the fluorescence intensity, detected in the tumor, linearly 
depends on the HER2 expression, measured ex vivo by an ELISA assay for the same 
tumor.
Biodegradable NIR gold nanoclusters: photo-acoustic imaging and in-vivo 
clearance 
Paper 7910-46 of Conference 7910
Date: Wednesday, 26 January 2011
Time: 10:40 AM – 11:00 AM
Author(s): Justina O. Tam, Avinash Murthy, Soon Joon Yoon, Stanislav Emelianov, 
Keith P. Johnston, The Univ. of Texas at Austin (United States); Konstantin V. 
Sokolov, The Univ. of Texas M.D. Anderson Cancer Ctr. (United States)
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Plasmonic nanoparticles have shown strong potential as NIR imaging and 
therapeutic agents. However, a major roadblock to clinical translation is their 
non-biodegradability, and thus potential for long term in vivo systemic 
toxicity. Here, we investigate in vivo clearance of gold nanoclusters, which are 
assemblies of sub-5nm gold spheres into sub-100nm clusters mediated by a 
biodegradable polymer. Nanocluster degradation in Balb/c mice was measured using 
neutron activation analysis (NAA) and dark-field reflectance (DR) imaging at 1 
day, 1 week, and 1 month after tail vein injection. Results showed degradation 
after 1 month and excretion of gold into feces and urine.
 
Del Mar Photonics - Newsletter Fall 2010 - Newsletter Winter 2010
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