Your search keyword '"Anand Giddabasappa"' showing total 9 results

1. Molecular imaging reveals biodistribution of P-cadherin LP-DART bispecific and trafficking of adoptively transferred T cells in mouse xenograft model

Author

Timothy Scott Fisher, Tracey Clark, Rand Norberg, Vijay Gupta, Chad May, Anand Giddabasappa, Justin Cohen, John David, and Adam Root

Subjects

Biodistribution, Bispecific antibody, biology, tumor targeting, Chemistry, CD3, T cells, molecular imaging, In vitro, bispecific antibody, Oncology, Mouse xenograft, In vivo, biology.protein, Cancer research, Cytotoxic T cell, Molecular imaging, biodistribution, human activities, Research Paper

Abstract

P-cadherin-LP-DART is a bispecific antibody targeting P-cadherin expressed on the tumor cells and CD3 on the T-cells. Previously we demonstrated the development and efficacy of P-cadherin-LP-DART in in vitro and in vivo models. Here, we evaluated the three pillars: exposure, targeting specificity and pharmacodynamic modulation for P-cadherin-LP-DART using fluorescence molecular tomography (FMT). Bispecific antibodies and T-cells were conjugated with a near-infrared fluorophores: VivoTag®680XL (VT680) and CellVue®NIR815 (CV815), respectively. In vitro binding and cytotoxic T-lymphocyte assay demonstrated that P-cadherin-LP-DART significantly retained its properties after VT680 conjugation. In vivo FMT imaging was performed to determine the bispecific biodistribution and T-cell trafficking in HCT-116 xenograft model. Peak tumor exposure (2.71%ID) was observed at 96 hr post-injection with measurable quantity even at 240 hr (1.46%ID) (Pillar 1). P-cadherin-LP-DART accumulation in tumor was 20-25 fold higher compared to Control-LP-DART demonstrating the targeting specificity (Pillar 2). Imaging after engraftment of CV815 labeled T-cells showed P-cadherin-LP-DART mediated T-cell trafficking in tumors (Pillar 3). This study harnessed the multichannel capability of FMT and demonstrated the targeting of drug and trafficking of T cells to tumors, simultaneously. Our results show the impact of molecular imaging in demonstrating three pillars of pharmacology, longitudinally and non-invasively.

Published

2020

2. Integrin αvβ8 on T cells suppresses anti-tumor immunity in multiple models and is a promising target for tumor immunotherapy

Author

Rosemary J. Akhurst, Bahar Zivak, Eswari Dodagatta-Marri, John T. Li, Niessen Kyle Steven, Bing Yang, Szu-Ying Chen, Joselyn S. Del Cid, Dean Sheppard, Michael Rosenblum, Benjia Liang, Dominique S. Meyer, Tatsuya Tsukui, Anand Giddabasappa, Hsiao-Yen Ma, Lauren Pinzas, Sharon Yang, Mark B. Headley, Kai-Hui Sun, Nilgun Isik Reed, Xin Ren, Joseph Dal Porto, Kavon Noorbehesht, Amha Atakilit, and Byron Hann

Subjects

CD4-Positive T-Lymphocytes, Male, Integrins, Antibodies, Neoplasm, medicine.medical_treatment, T-Lymphocytes, Mice, Transgenic, CD8-Positive T-Lymphocytes, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Granzymes, Lymphocyte Depletion, Article, Interferon-gamma, Mice, Tumor Necrosis Factor Receptor Superfamily, Member 9, Cancer immunotherapy, Transforming Growth Factor beta, Cell Line, Tumor, Neoplasms, medicine, Tumor Microenvironment, Cytotoxic T cell, Animals, CTLA-4 Antigen, IL-2 receptor, Smad3 Protein, Cell Proliferation, Chemistry, Immunity, Cancer, Immunotherapy, medicine.disease, Survival Analysis, Granzyme B, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, Mutation, Cancer research, CD8, Transforming growth factor, Signal Transduction, T-Lymphocytes, Cytotoxic

Abstract

SUMMARY αvβ8 integrin, a key activator of transforming growth factor β (TGF-β), inhibits anti-tumor immunity. We show that a potent blocking monoclonal antibody against αvβ8 (ADWA-11) causes growth suppression or complete regression in syngeneic models of squamous cell carcinoma, mammary cancer, colon cancer, and prostate cancer, especially when combined with other immunomodulators or radiotherapy. αvβ8 is expressed at the highest levels in CD4+CD25+ T cells in tumors, and specific deletion of β8 from T cells is as effective as ADWA-11 in suppressing tumor growth. ADWA-11 increases expression of a suite of genes in tumor-infiltrating CD8+ T cells normally inhibited by TGF-β and involved in tumor cell killing, including granzyme B and interferon-γ. The in vitro cytotoxic effect of tumor CD8 T cells is inhibited by CD4+CD25+ cells, and this suppressive effect is blocked by ADWA-11. These findings solidify αvβ8 integrin as a promising target for cancer immunotherapy., Graphical abstract, In brief TGF-β suppresses anti-tumor immunity. Dodagatta-Marri, Ma et al. show that the TGF-β-activating integrin αvβ8 is expressed on CD25+CD4+ tumor T cells and suppresses anti-tumor immunity by CD8+ T cells. Blocking this integrin enhances tumor cell killing and synergizes with multiple immune modulators or radiotherapy to induce long-term anti-tumor immunity.

Published

2020

3. Assessment of near-infrared fluorophores to study the biodistribution and tumor targeting of an IL13 receptor α2 antibody by fluorescence molecular tomography

Author

Christopher T. Winkelmann, Rachel Roach, Dangshe Ma, Lindsay King, Mauricio Leal, Mary E. Spilker, Antonio Esparza, Cedo M. Bagi, Parul Gupta, Jo-Ann Wentland, and Anand Giddabasappa

Subjects

0301 basic medicine, Biodistribution, Pathology, medicine.medical_specialty, Fluorophore, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, In vivo, medicine, biotherapeutics, fluorescence molecular tomography (FMT), biodistribution, tumor targeting, Chemistry, molecular imaging, Molecular biology, In vitro, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Molecular imaging, Ex vivo, Preclinical imaging, Research Paper

Abstract

// Parul Gupta 1 , Jo-Ann Wentland 2 , Mauricio Leal 2 , Dangshe Ma 3, 6 , Rachel Roach 4 , Antonio Esparza 5 , Lindsay King 2 , Mary E. Spilker 2 , Cedo Bagi 1 , Christopher T. Winkelmann 1 and Anand Giddabasappa 1 1 Global Science and Technology, Comparative Medicine, Pfizer, Inc., La Jolla, CA, USA 2 Pharmacokinetics and Drug Metabolism, Pfizer, Inc., New York NY, USA 3 Oncology Research Unit, Pfizer, Inc., Pearl River, NY, USA 4 Center for Therapeutic Innovation, Pfizer, Inc., La Jolla, CA, USA 5 Comparative Medicine, Pfizer, Inc., La Jolla, CA, USA 6 Current affiliation: Regeneron Pharmaceuticals, Tarrytown, NY, USA Correspondence to: Anand Giddabasappa, email: anand.giddabasappa@pfizer.com Keywords: biotherapeutics, tumor targeting, biodistribution, fluorescence molecular tomography (FMT), molecular imaging Received: January 16, 2017 Accepted: July 03, 2017 Published: July 26, 2017 ABSTRACT Non-invasive imaging using radiolabels is a common technique used to study the biodistribution of biologics. Due to the limited shelf-life of radiolabels and the requirements of specialized labs, non-invasive optical imaging is an attractive alternative for preclinical studies. Previously, we demonstrated the utility of fluorescence molecular tomography (FMT) an optical imaging modality in evaluating the biodistribution of antibody-drug conjugates. As FMT is a relatively new technology, few fluorophores have been validated for in vivo imaging. The goal of this study was to characterize and determine the utility of near-infrared (NIR) fluorophores for biodistribution studies using interleukin-13 receptor subunit alpha-2 antibody (IL13Rα2-Ab). Eight fluorophores ( ex/em : 630/800 nm) with an N-hydroxysuccinimide (NHS) linker were evaluated for Ab conjugation. The resulting antibody-fluorophore (Ab-F) conjugates were evaluated in vitro for degree of conjugation, stability and target-binding, followed by in vivo / ex vivo FMT imaging to determine biodistribution in a xenograft model. The Ab-F conjugates (except Ab-DyLight800) showed good in vitro stability and antigen binding. All Ab-F conjugates (except for Ab-BOD630) resulted in a quantifiable signal in vivo and had similar biodistribution profiles, with peak tumor accumulation between 6 and 24 h post-injection. In vivo / ex vivo FMT imaging showed 17–34% ID/g Ab uptake by the tumor at 96 h. Overall, this is the first study to characterize the biodistribution of an Ab using eight NIR fluorophores. Our results show that 3-dimensional optical imaging is a valuable technology to understand biodistribution and targeting, but a careful selection of the fluorophore for each Ab is warranted.

Published

2017

4. Axitinib inhibits retinal and choroidal neovascularization in in vitro and in vivo models

Author

Hovhannes J. Gukasyan, David Paterson, Karen J. Klamerus, Kush Lalwani, Ronald A. Schachar, Anand Giddabasappa, Lydia Mosyak, Rand Norberg, Kay D. Rittenhouse, and Jeetendra Eswaraka

Subjects

Male, 0301 basic medicine, Platelet-derived growth factor, Axitinib, genetic structures, Tyrosine-kinase inhibitor, Neovascularization, chemistry.chemical_compound, 0302 clinical medicine, Wet age-related macular degeneration, Medicine, 3D co-culture model, Fluorescein Angiography, In vitro angiogenesis, biology, Imidazoles, Immunohistochemistry, Sensory Systems, Choroidal neovascularization, Intravitreal Injections, Rat choroidal neovascularization, medicine.symptom, Platelet-derived growth factor receptor, medicine.drug, medicine.medical_specialty, Indazoles, medicine.drug_class, 03 medical and health sciences, Cellular and Molecular Neuroscience, In vivo, Internal medicine, Small molecule receptor tyrosine kinase inhibitor, Animals, Humans, Protein Kinase Inhibitors, Aged, Cell Proliferation, business.industry, Endothelial Cells, Mesenchymal Stem Cells, Macular degeneration, medicine.disease, Choroidal Neovascularization, eye diseases, Rats, Disease Models, Animal, Ophthalmology, 030104 developmental biology, Endocrinology, chemistry, 030221 ophthalmology & optometry, biology.protein, Cancer research, sense organs, Pericytes, business

Abstract

Age-related Macular Degeneration (AMD) is the leading cause of visual impairment and blindness in the elderly in developed countries. Neovascular/exudative (wet) AMD is the aggressive form of AMD and can involve choroidal neovascularization and vascular leakage. Anti-vascular endothelial growth factor (anti-VEGF) medications have significantly improved treatment of wet-AMD. However, only approximately 40% of patients obtain full benefit from anti-VEGF therapy and the medications are given by intravitreal injection. Axitinib, a small molecule multi-receptor tyrosine kinase inhibitor used for the treatment of advanced renal cell carcinoma, is taken orally and inhibits VEGF activity by blocking VEGF receptors. Axitinib also has the advantage of blocking platelet derived growth factor (PDGF) receptors which play a role in neovascularization. Using in vitro human retinal microvascular endothelial cells (HRMVECs), human brain vascular pericytes (HBVRs), 3D co-culture vessel sprout assay, and in vivo laser induced rat choroidal neovascularization (CNV) models, the effect of axitinib on neovascularization was evaluated. Axitinib inhibited neovascularization better than anti-VEGF and/or anti-hPDGF-B mAb in the in vitro models demonstrating that combined inhibition of both VEGF and PDGF pathways may be synergistic in treating wet-AMD. Additionally, axitinib showed good efficacy at a low dose (0.875 mg/day) in laser-induced CNV model in rats. In conclusion our data shows that axitinib, an inhibitor of VEGF and PDGF-B pathways may be useful in ameliorating wet-AMD therapy.

Published

2016

5. Abstract B25: Development of a nanoparticle containing the PI3K/mTOR dual Inhibitor, gedatolisib, for cancer therapy

Author

Jennifer Lafontaine, Valeria Fantin, Anand Giddabasappa, Zhenxiong Wang, Wenhu Huang, Shubha Bagrodia, Susan Low, Hui Wang, Louise Cadzow, Young-Ho Song, Gabriel Troche, Ravi Visswanathan, Robert T. Abraham, Greg Troiano, Mary E. Spilker, and Lianglin Zhang

Subjects

Cancer Research, business.industry, Cmax, medicine.disease, Tumor antigen, chemistry.chemical_compound, Prostate cancer, Therapeutic index, medicine.anatomical_structure, Oncology, chemistry, Prostate, Cancer research, medicine, Enzalutamide, business, Lung cancer, Molecular Biology, PI3K/AKT/mTOR pathway

Abstract

Gedatolisib, a PI3K/mTOR dual inhibitor delivered intravenously, is in early clinical trials in women with metastatic ER+ breast cancer. We reasoned that the therapeutic index could be further maximized by encapsulation of gedatolisib in nanoparticles (NP), thereby providing longer half-life, sustained release, blunting of Cmax and associated toxicity, asymmetric distribution to leaky tumor vasculature and the possibility of less frequent dosing. PF-07034663 is a polymeric NP encapsulating gedatolisib, targeted to prostate-specific membrane antigen (PSMA), a clinically validated tumor antigen expressed on prostate cancer cells and the neovasculature of some nonprostate solid tumors. Studies in mice, rats, and cynomolgus monkeys demonstrated that the terminal half-life of PF-07034663 following intravenous administration increased by ~1.5 fold and the Cmax of released gedatolisib from PF-07034663 decreased by ~75 fold compared to gedatolisib delivered by the same route. Gedatolisib released from PF-07034663 exhibited markedly enhanced intratumoral accumulation compared to gedatolisib (~40 fold), indicating enhanced tissue delivery and/or prolonged retention. In exploratory toxicology studies, PF-07034663 caused no hyper-insulinemic spike in rats, in contrast to gedatolisib. To evaluate the antitumor activity of PF-07034663, we performed tumor growth inhibition (TGI) studies in PSMA-positive C4-2 prostate and in PSMA-negative MDAMB361 ER+ breast and A549 lung xenograft tumor models. In the C4-2 model, PF-07034663 showed dose-dependent antitumor efficacy as a single agent, and, in combination with enzalutamide, exhibited enhanced activity leading to tumor regressions. PF 07034663 also exhibited prolonged, dose-dependent inhibition of phosphorylation of S6 (pS6) in the C4-2 model compared to gedatolisib. Interestingly, increased pharmacodynamics (PD) responses compared to gedatolisib were not restricted to PSMA-positive tumors. Moreover, TGI responses were increased in the PSMA-negative A549 lung cancer model, relative to those observed with gedatolisib. PF 07034663 treatment in spontaneous prostate tumors in PTENnullp53mut GEM mice and in subcutaneous allografts of these spontaneous tumors in wild-type mice showed that treatment of PF-07034663 caused similar pS6 inhibition in both models, suggesting that PD modulation is independent of tumor origin or milieu and is less likely due to altered enhanced permeability and retention (EPR) effect. Taken together, PF-07034663 exhibits potential for improved tolerability, sustained tumor PK, prolonged PD modulation, and less frequent dosing schedule compared to gedatolisib. These results support further exploration of gedatolisib in tumor-targeted or non-tumor-targeted nanoparticles in clinical trials as a promising vehicle for delivery of PI3K/mTOR inhibitors to advanced cancer patients. Citation Format: Lianglin Zhang, Gabriel Troche, Ravi Visswanathan, Wenhu Huang, Young-Ho Song, Mary E. Spilker, Zhenxiong Wang, Hui Wang, Anand Giddabasappa, Louise Cadzow, Susan Low, Greg Troiano, Jennifer Lafontaine, Valeria Fantin, Robert T. Abraham, Shubha Bagrodia. Development of a nanoparticle containing the PI3K/mTOR dual Inhibitor, gedatolisib, for cancer therapy [abstract]. In: Proceedings of the AACR Special Conference on Targeting PI3K/mTOR Signaling; 2018 Nov 30-Dec 8; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Res 2020;18(10_Suppl):Abstract nr B25.

Published

2020

6. Editor's Highlight: Plasma miR-183/96/182 Cluster and miR-124 are Promising Biomarkers of Rat Retinal Toxicity

Author

Anand Giddabasappa, Qinghai Peng, Wenhu Huang, Walter Collette, Michelle Twamley, Dalia Kalabat, John David, and Shirley A. Aguirre

Subjects

0301 basic medicine, Oncology, Male, medicine.medical_specialty, Pathology, Biology, Toxicology, Retina, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, microRNA, Toxicity Tests, medicine, Electroretinography, Animals, Rats, Wistar, Retinal, Rats, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Choroidal neovascularization, chemistry, Drug development, Biomarker (medicine), Histopathology, Female, sense organs, medicine.symptom, Erg, Biomarkers

Abstract

Retinal toxicity is one of the leading causes of attrition in drug development, and drug-induced retinal toxicity remains an issue in both drug discovery and postmarketed drugs. Derisking strategies to help with early identification of retinal injury utilizing a predictive retinal miRNA biomarker would greatly benefit decision-making in drug discovery programs, ultimately reducing attrition due to retinal toxicity. Our previous work demonstrated elevation of circulating retina-enriched miRNAs in a retinal toxicity model. To further validate our previous observation, 2 additional rat retinal injury models were utilized in this study: NaIO3-induced retinal injury and laser-induced choroidal neovascularization (CNV) injury model. Following induction of retina tissue injuries, circulating miR-183/96/182 cluster (miR-183 cluster), and miR-124 was investigated, as well as evaluations using an electroretinogram (ERG) and histopathology analysis. Data revealed that circulating miR-183/96/182 cluster was significantly increased (2- to 15-fold) compared with baseline/control in both laser-induced CNV and NaIO3-induced retinal injury models. Moreover, the severity of the retinal injury evaluated by ERG and histopathology correlated highly with elevation of these retina-enriched miRNAs in plasma. MiR-124 was also significantly increased in comparison with baseline/control by ∼25-fold postrepeat-doses of 30 mg/kg NaIO3 treatment. Increased level of these plasma miRNA biomarkers appeared to be dose- and time-dependent upon NaIO3 or laser treatment. The results suggest that the retina-enriched miRNAs (miR-183/96/182 cluster and miR-124) could serve as convenient and predictive biomarkers of retinal toxicity in drug development.

Published

2016

7. Biodistribution and Targeting of Anti-5T4 Antibody-Drug Conjugate Using Fluorescence Molecular Tomography

Author

Mary E. Spilker, Rand Norberg, Mauricio Leal, Vijay Gupta, Parul Gupta, Anand Giddabasappa, Jeetendra Eswaraka, Jo-Ann Wentland, Puja Sapra, and Brian Rago

Subjects

0301 basic medicine, Cancer Research, Biodistribution, Antibody-drug conjugate, Immunoconjugates, Antineoplastic Agents, Fluorescence, 03 medical and health sciences, Mice, 0302 clinical medicine, Pharmacokinetics, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Tissue Distribution, Membrane Glycoproteins, medicine.diagnostic_test, Chemistry, Xenograft Model Antitumor Assays, Molecular Imaging, Tumor Burden, Disease Models, Animal, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Biophysics, Molecular imaging, Tomography, X-Ray Computed, Preclinical imaging, Ex vivo, Emission computed tomography, Conjugate

Abstract

Understanding a drug's whole-body biodistribution and tumor targeting can provide important information regarding efficacy, safety, and dosing parameters. Current methods to evaluate biodistribution include in vivo imaging technologies like positron electron tomography and single-photon emission computed tomography or ex vivo quantitation of drug concentrations in tissues using autoradiography and standard biochemical assays. These methods use radioactive compounds or are cumbersome and do not give whole-body information. Here, for the first time, we show the utility of fluorescence molecular tomography (FMT) imaging to determine the biodistribution and targeting of an antibody–drug conjugate (ADC). An anti–5T4-antibody (5T4-Ab) and 5T4-ADC were conjugated with a near-infrared (NIR) fluorophore VivoTag 680XL (VT680). Both conjugated compounds were stable as determined by SEC-HPLC and plasma stability studies. Flow cytometry and fluorescence microscopy studies showed that VT680-conjugated 5T4-ADC specifically bound 5T4-expressing cells in vitro and also exhibited a similar cytotoxicity profile as the unconjugated 5T4-ADC. In vivo biodistribution and tumor targeting in an H1975 subcutaneous xenograft model demonstrated no significant differences between accumulation of VT680-conjugated 5T4-Ab or 5T4-ADC in either normal tissues or tumor. In addition, quantitation of heart signal from FMT imaging showed good correlation with the plasma pharmacokinetic profile suggesting that it (heart FMT imaging) may be a surrogate for plasma drug clearance. These results demonstrate that conjugation of VT680 to 5T4-Ab or 5T4-ADC does not change the behavior of native biologic, and FMT imaging can be a useful tool to understand biodistribution and tumor-targeting kinetics of antibodies, ADCs, and other biologics. Mol Cancer Ther; 15(10); 2530–40. ©2016 AACR.

Published

2015

8. Abstract 2861: Dose-dependent tissue distribution and tumor targeting of Notch3-ADC using fluorescence molecular tomography imaging

Author

Mauricio Leal, Bing Yang, Parul Gupta, Kenneth G. Geles, Anand Giddabasappa, Fengping Li, Jonathan Golas, Christopher T. Winkelmann, and Antonio Esparza

Subjects

Cancer Research, Biodistribution, medicine.medical_specialty, Antibody-drug conjugate, Chemistry, body regions, Oncology, Cancer stem cell, In vivo, Cancer cell, Cancer research, medicine, Immunohistochemistry, Radiology, Preclinical imaging, Ex vivo

Abstract

Background: NOTCH3, a cell surface receptor involved in cell-cell communications, is over-expressed or amplified in certain human tumors. NOTCH3 is known to regulate proliferation, differentiation and survival of cancer cells or cancer stem cells and thus an important therapeutic target. NOTCH3 antibody drug conjugate (ADC) is comprised of humanized anti-NOTCH3 antibody conjugated to an auristatin based cytotoxic payload. NOTCH3-ADC has shown promising results in pre-clinical tumor models. In this study we evaluated the kinetics, dose-dependent tissue distribution, tumor accumulation and targeting specificity of the NOTCH3-ADC in OVCAR3 xenograft model using fluorescence molecular tomography (FMT) imaging. The NOTCH3-ADC is mouse cross-reactive thus providing an accurate assessment of biodistribution. Methods: NOTCH3-ADC was conjugated to the near-infrared dye, AlexaFluor680 (AF680). The in vitro cellular binding was evaluated by cell-based ELISA. In vivo biodistribution was evaluated using OVCAR3 subcutaneous xenograft model. NOTCH3-ADC-AF680 (1mg/kg; 3mg/kg and 10mg/kg) was injected when the tumors were ~300mm3 and imaged 5 min, 24, 48, 96, 168 and 240 h post-injection. Ex vivo FMT imaging, pharmacokinetic analysis and immunohistochemistry (IHC) was performed at 48 and 240 h after whole-body perfusion. An in vivo receptor competition FMT study was performed by injecting excess of unconjugated anti-NOTCH3 antibody (Ab) or a non-targeted control Ab. Results: In vitro cell binding studies showed that conjugation of AF680 to NOTCH3-ADC did not change its binding ability. A dose-dependent tumor regression was also observed after a single injection of NOTCH3-ADC-AF680. In vivo FMT imaging showed dose-dependent whole-body clearance kinetics of NOTCH3-ADC. Dose-dependent accumulation in the tumors was observed with peak accumulation at 24-48 h post-injection and a slow decline at later time-points. A maximum accumulation of ~10 %ID/g was observed which was independent of the dose of NOTCH3-ADC-AF680. Ex vivo FMT quantitation of tumor was consistent with the IHC for antibody and LC/MS analysis of released payload. Pharmacological competition with excess unlabeled control Ab did not block tumor accumulation of NOTCH3-ADC-AF680, whereas excess unlabeled NOTCH3-Ab blocked ~47% of NOTCH3-ADC-AF680 accumulation. There was no significant specific accumulation of NOTCH3-ADC in other organs as observed by FMT imaging or IHC. Conclusions: These imaging studies provided understanding of the kinetics, tumor accumulation and biodistribution of NOTCH3-ADC. Further this work showcase the utility of non-invasive FMT imaging in better understanding of pharmacology and behavior of biologic drugs. Citation Format: Anand Giddabasappa, Parul Gupta, Mauricio Leal, Jonathan Golas, Fengping Li, Bing Yang, Antonio Esparza, Christopher Winkelmann, Kenneth Geles. Dose-dependent tissue distribution and tumor targeting of Notch3-ADC using fluorescence molecular tomography imaging [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 2861. doi:10.1158/1538-7445.AM2017-2861

Published

2017

9. Abstract 5111: Bio-distribution and tumor targeting of a P-cadherin x CD3 bi-specific redirected T-cell molecule using fluorescence molecular tomography imaging

Author

Norberg Rand, John David, Tracey Clark, Rohner Allison Karlyn, Vijay Gupta, Chad May, Justin Cohen, Adam Root, Nahor Haddish-Berhane, Timothy Scott Fisher, and Anand Giddabasappa

Subjects

Cancer Research, Pathology, medicine.medical_specialty, biology, medicine.diagnostic_test, Chemistry, T cell, CD3, Cell, Molecular biology, Flow cytometry, medicine.anatomical_structure, Oncology, In vivo, medicine, biology.protein, Cytotoxic T cell, human activities, Ex vivo, Binding domain

Abstract

Introduction: Previously we have shown the utility of Fluorescent Molecular Tomography (FMT) imaging in evaluating bio-distribution of biologics. P-cadherin LP-DART is a bi-specific Dual Affinity Re-Targeting (DART®) molecule targeting CD3 expressed on T-cells and P-cadherin expressed on tumors. In this study we evaluated the bio-distribution and tumor targeting of P-cadherin LP-DART using FMT imaging in a colorectal xenograft model. Methods: NSG or athymic nude mice with subcutaneous HCT-116 xenografts were used. Studies that included engraftment of T-cells received either PBMNCs or T-cells isolated from healthy human volunteers. Bio-distribution studies were initiated when the tumors reached 300-500 mm3. P-cadherin LP-DART or a negative control-DART (non-targeted domain x CD3 binding domain) was conjugated with a near-infrared fluorophore VivoTag680XL (VT680), and the labeling efficiency was determined by spectrophotometer. T-cells used in trafficking studies were labeled with CellVue815. Cell surface P-cadherin expression and P-cadherin LP-DART binding was determined by flow cytometry. T-cell activity was measured with cytotoxic T-lymphocyte (CTL) assays. FMT imaging was performed longitudinally post injection of labeled bi-specifics. Data was analyzed using TrueQuant software. Plasma and tissues were collected for PK analysis by ELISA or histology. Results: VT680 conjugation to P-cadherin LP-DART did not significantly affect the binding to P-cadherin, whereas CD3 binding was decreased. In vivo FMT imaging revealed high levels of P-cadherin LP-DART accumulation in the tumors. The in vivo kinetics revealed that the peak accumulation in tumors was 96hrs post-injection. At 240hrs post-injection, there was still measurable P-cadherin LP-DART detected in tumors. Ex vivo imaging showed 20-25 fold increase in accumulation of P-cadherin LP-DART compared to negative control DART. Comparison of P-cadherin LP-DART accumulation between PBMNC engrafted and non-engrafted model showed no significant difference in quantity or kinetics. There was no significant difference in the kinetics of elimination in the whole-body, heart or liver between P-cadherin LP-DART or negative control. Ex vivo comparison of accumulation in various organs showed no difference between P-cadherin LP-DART or negative control. Cell trafficking studies with CellVue labeled T-cells showed the co-localization of T-cells and P-cadherin LP-DART in tumors. Conclusion: FMT imaging showed that P-cadherin LP-DART specifically targeted HCT-116 tumors. Cell trafficking studies showed that engrafted T-cells accumulated in tumors. This study shows the utility of FMT in bio-distribution studies of biologics and in vivo cell trafficking. Citation Format: Anand Giddabasappa, Vijay Gupta, Timothy S. Fisher, John David, Norberg Rand, Allison Rohner, Justin Cohen, Tracey Clark, Nahor Haddish-Berhane, Adam Root, Chad May. Bio-distribution and tumor targeting of a P-cadherin x CD3 bi-specific redirected T-cell molecule using fluorescence molecular tomography imaging. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 5111. doi:10.1158/1538-7445.AM2015-5111

Published

2015