Your search keyword '"Blesida Punzalan"' showing total 40 results

1. Data from Intraperitoneal Pretargeted Radioimmunotherapy for Colorectal Peritoneal Carcinomatosis

Author

Sarah M. Cheal, Steven M. Larson, Nai Kong V. Cheung, Neeta Pandit-Taskar, Achim Jungbluth, Andrea Cercek, Garrett M. Nash, Sébastien Monette, Pat B. Zanzonico, Brian H. Santich, Hong-fen Guo, Hong Xu, Mitesh Patel, Daniela Burnes Vargas, Blesida Punzalan, Edward K. Fung, Darren R. Veach, Sebastian K. Chung, Meghan M. Bell, and Christopher S. Chandler

Abstract

Peritoneal carcinomatosis (PC) is considered incurable, and more effective therapies are needed. Herein we test the hypothesis that GPA33-directed intracompartmental pretargeted radioimmunotherapy (PRIT) can cure colorectal peritoneal carcinomatosis. Nude mice were implanted intraperitoneally with luciferase-transduced GPA33-expressing SW1222 cells for aggressive peritoneal carcinomatosis (e.g., resected tumor mass 0.369 ± 0.246 g; n = 17 on day 29). For GPA33-PRIT, we administered intraperitoneally a high-affinity anti-GPA33/anti-DOTA bispecific antibody (BsAb), followed by clearing agent (intravenous), and lutetium-177 (Lu-177) or yttrium-86 (Y-86) radiolabeled DOTA-radiohapten (intraperitoneal) for beta/gamma-emitter therapy and PET imaging, respectively. The DOTA-radiohaptens were prepared from S-2-(4-aminobenzyl)-1,4,7, 10-tetraazacyclododecane tetraacetic acid chelate (DOTA-Bn). Efficacy and toxicity of single- versus three-cycle therapy were evaluated in mice 26–27 days post-tumor implantation. Single-cycle treatment ([177Lu]LuDOTA-Bn 111 MBq; tumor dose: 4,992 cGy) significantly prolonged median survival (MS) approximately 2-fold to 84.5 days in comparison with controls (P = 0.007). With three-cycle therapy (once weekly, total 333 MBq; tumor dose: 14,975 cGy), 6/8 (75%) survived long-term (MS > 183 days). Furthermore, for these treated long-term survivors, 1 mouse was completely disease free (microscopic “cure”) at necropsy; the others showed stabilized disease, which was detectable during PET-CT using [86Y]DOTA-Bn. Treatment controls had MS ranging from 42–52.5 days (P < 0.001) and 19/20 mice succumbed to progressive intraperitoneal disease by 69 days. Multi-cycle GPA33 DOTA-PRIT significantly prolongs survival with reversible myelosuppression and no chronic marrow (929 cGy to blood) or kidney (982 cGy) radiotoxicity, with therapeutic indices of 12 for blood and 12 for kidneys. MTD was not reached.

Published

2023

2. Supplementary Data from Intraperitoneal Pretargeted Radioimmunotherapy for Colorectal Peritoneal Carcinomatosis

Author

Sarah M. Cheal, Steven M. Larson, Nai Kong V. Cheung, Neeta Pandit-Taskar, Achim Jungbluth, Andrea Cercek, Garrett M. Nash, Sébastien Monette, Pat B. Zanzonico, Brian H. Santich, Hong-fen Guo, Hong Xu, Mitesh Patel, Daniela Burnes Vargas, Blesida Punzalan, Edward K. Fung, Darren R. Veach, Sebastian K. Chung, Meghan M. Bell, and Christopher S. Chandler

Abstract

Supplementary Data

Published

2023

3. Intraperitoneal Pretargeted Radioimmunotherapy for Colorectal Peritoneal Carcinomatosis

Author

Garrett M. Nash, Blesida Punzalan, Sebastien Monette, Meghan Bell, Neeta Pandit-Taskar, Christopher Chandler, Edward K Fung, Sarah M. Cheal, Hong Xu, Daniela Burnes Vargas, Nai-Kong V. Cheung, Andrea Cercek, Sebastian K Chung, Hong-fen Guo, Brian H. Santich, Achim A. Jungbluth, Steven M. Larson, Darren R. Veach, Mitesh Patel, and Pat Zanzonico

Subjects

Cancer Research, Bispecific antibody, medicine.medical_specialty, Kidney, business.industry, Urology, Mice, Nude, Once weekly, Pet imaging, Radioimmunotherapy, Article, Peritoneal carcinomatosis, Disease Models, Animal, Mice, medicine.anatomical_structure, Oncology, Toxicity, Animals, Humans, Medicine, Pretargeted Radioimmunotherapy, Colorectal Neoplasms, business, Peritoneal Neoplasms, Median survival

Abstract

Peritoneal carcinomatosis (PC) is considered incurable, and more effective therapies are needed. Herein we test the hypothesis that GPA33-directed intracompartmental pretargeted radioimmunotherapy (PRIT) can cure colorectal peritoneal carcinomatosis. Nude mice were implanted intraperitoneally with luciferase-transduced GPA33-expressing SW1222 cells for aggressive peritoneal carcinomatosis (e.g., resected tumor mass 0.369 ± 0.246 g; n = 17 on day 29). For GPA33-PRIT, we administered intraperitoneally a high-affinity anti-GPA33/anti-DOTA bispecific antibody (BsAb), followed by clearing agent (intravenous), and lutetium-177 (Lu-177) or yttrium-86 (Y-86) radiolabeled DOTA-radiohapten (intraperitoneal) for beta/gamma-emitter therapy and PET imaging, respectively. The DOTA-radiohaptens were prepared from S-2-(4-aminobenzyl)-1,4,7, 10-tetraazacyclododecane tetraacetic acid chelate (DOTA-Bn). Efficacy and toxicity of single- versus three-cycle therapy were evaluated in mice 26–27 days post-tumor implantation. Single-cycle treatment ([177Lu]LuDOTA-Bn 111 MBq; tumor dose: 4,992 cGy) significantly prolonged median survival (MS) approximately 2-fold to 84.5 days in comparison with controls (P = 0.007). With three-cycle therapy (once weekly, total 333 MBq; tumor dose: 14,975 cGy), 6/8 (75%) survived long-term (MS > 183 days). Furthermore, for these treated long-term survivors, 1 mouse was completely disease free (microscopic “cure”) at necropsy; the others showed stabilized disease, which was detectable during PET-CT using [86Y]DOTA-Bn. Treatment controls had MS ranging from 42–52.5 days (P < 0.001) and 19/20 mice succumbed to progressive intraperitoneal disease by 69 days. Multi-cycle GPA33 DOTA-PRIT significantly prolongs survival with reversible myelosuppression and no chronic marrow (929 cGy to blood) or kidney (982 cGy) radiotoxicity, with therapeutic indices of 12 for blood and 12 for kidneys. MTD was not reached.

Published

2022

4. Data from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Purpose:Abnormal Notch signaling promotes cancer cell growth and tumor progression in various cancers. Targeting γ-secretase, a pivotal regulator in the Notch pathway, has yielded numerous γ-secretase inhibitors (GSIs) for clinical investigation in the last 2 decades. However, GSIs have demonstrated minimal success in clinical trials in part due to the lack of specific and precise tools to assess γ-secretase activity and its inhibition in vivo.Experimental Design:We designed an imaging probe based on GSI Semagacestat structure and synthesized the radioiodine-labeled analogues [131I]- or [124I]-PN67 from corresponding trimethyl-tin precursors. Both membrane- and cell-based ligand-binding assays were performed using [131I]-PN67 to determine the binding affinity and specificity for γ-secretase in vitro. Moreover, we evaluated [124I]-PN67 by PET imaging in mammary tumor and glioblastoma mouse models.Results:The probe was synthesized through iodo-destannylation using chloramine-T as an oxidant with a high labeling yield and efficiency. In vitro binding results demonstrate the high specificity of this probe and its ability for target replacement study by clinical GSIs. PET imaging studies demonstrated a significant (P < 0.05) increased in the uptake of [124I]-PN67 in tumors versus blocking or sham control groups across multiple mouse models, including 4T1 allograft, MMTV-PyMT breast cancer, and U87 glioblastoma allograft. Ex vivo biodistribution and autoradiography corroborate these results, indicating γ-secretase specific tumor accumulation of [124I]-PN67.Conclusions:[124I]-PN67 is a novel PET imaging agent that enables assessment of γ-secretase activity and target engagement of clinical GSIs.

Published

2023

5. Figure S1 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Figure 1. The radiolabeling product of [124I]PN67 was confirmed by co-injecting cold compound 2 (100uM in 100ul DMSO/H2O/MeCN) with the radioactive fraction (50uCi in 100ul H2O/MeCN) onto HPLC. (A) UV 235/254nm wavelength channels were used to detect absorption of cold PN67. Retention time (RT): 8.17min; (B) The radioactivity was detected by a bioscan flow-count detector. Retention time (RT): 8.28min. Radiochemical purity (>99%) was calculated based on integration of area under curve. The bioscan peak is slightly delayed compared with UV signal because of instrument setting.

Published

2023

6. Table S1 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Table 1. Biodistribution data of [124I]PN67 versus time/h, administrated by i.v. tail-vein injection in BALB/c mice bearing 4T1-Luc tumors. Data is represented as average %ID/g {plus minus} SD with n=5 animals/group.

Published

2023

7. Figure S5 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Figure 5. γ-Secretase activity of different mouse tissues. The membrane fractions of tissues were prepared to determine γ-secretase activity. (n=4)

Published

2023

8. Figure S2 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Figure 2. (A) Representative bioluminescent images (left panels) and PET images (right panels) of mice bearing 4T1-Luc tumor. The bioluminescent image was taken 1h prior to PET experiment, whereas PET images at 2 h post injection was shown. Blocking was carried out by co-injecting of 1 at 30mg/kg with the tracer. (B) PET quantitation of [124I]-PN67 uptake in 4T1-Luc tumors vs. blocking condition (1, 30 mg/kg). Muscle uptake was quantified to gauge the level of background signal. Data are average %ID/g {plus minus} SD (n = 4). %ID/g = percentage injected dose per gram, **P < 0.01. (C) Representative autoradiography of 4T1-Luc tumors from (A).

Published

2023

9. Figure S4 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Figure 4. Representative MR imaging of U87 glioblastoma mouse model (top panel) versus sham control group (bottom panel).

Published

2023

10. NMR and HRMS from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

NMR and Mass (HRMS) spectroscopy data

Published

2023

11. Figure S3 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Figure 3. Representative PET imaging of endogenously developed mammary tumors from MMTVPyMT transgenic mice using [124I]PN67. The tumor location was indicated by red cycles. PET imaging studies were performed at 2h post-injection on a microPET scanner with (bottom panel) or without (top panel) blocking inhibitor (1, 30mg/kg).

Published

2023

12. Table S2 from Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

Yue-Ming Li, Naga Vara Kishore Pillarsetty, Jason S. Lewis, Lukas M. Carter, Blesida Punzalan, Kelly E. Henry, Georgia Frost, George P. Liao, Thomas Li, Xianzhong Wu, Veronica L. Nagle, Teja Kalidindi, and Pengju Nie

Abstract

Supplementary Table 2. Biodistribution data of [124I]PN67 in non-tumor bearing BALB/c mice at 2h time point post injection. Data is represented as average %ID/g {plus minus} SD with n=5 animals/group.

Published

2023

13. Synthesis and evaluation of a bivalent radiohapten for DOTA-based pretargeted radioimmunotherapy

Author

Darren Veach, Brett Vaughn, Daniela Burnes Vargas, Shin Seo, Blesida Punzalan, Hong Xu, Hong-fen Guo, Simone Krebs, Guangbin Yang, Ouathek Ouerfelli, Nai-Kong Cheung, Steven Larson, and Sarah Cheal

Subjects

Cancer Research, Molecular Medicine, Radiology, Nuclear Medicine and imaging

Published

2022

14. Engineered Cells as a Test Platform for Radiohaptens in Pretargeted Imaging and Radioimmunotherapy Applications

Author

Michael R. McDevitt, Sarah M. Cheal, Brian H. Santich, Blesida Punzalan, Darren R. Veach, Simone Krebs, Guangbin Yang, Sebastien Monette, Thomas Z. Kubik, Lukas M. Carter, Steven M. Larson, Megan M. Dacek, Daniela Burnes Vargas, Nai-Kong V. Cheung, Ouathek Ouerfelli, David A. Scheinberg, and Adam Kesner

Subjects

Biodistribution, medicine.medical_treatment, Biomedical Engineering, Pharmaceutical Science, Bioengineering, 02 engineering and technology, 01 natural sciences, Article, Mice, Positron Emission Tomography Computed Tomography, medicine, Dosimetry, Animals, Humans, Tissue Distribution, neoplasms, Cell Engineering, Pretargeting, Pharmacology, 010405 organic chemistry, Chemistry, Organic Chemistry, HEK 293 cells, Radioimmunotherapy, 021001 nanoscience & nanotechnology, Xenograft Model Antitumor Assays, 0104 chemical sciences, HEK293 Cells, Test platform, Autoradiography, Radiopharmaceuticals, 0210 nano-technology, Haptens, Preclinical imaging, Ex vivo, Biotechnology, Biomedical engineering

Abstract

Pretargeted imaging and radioimmunotherapy approaches are designed to have superior targeting properties over directly targeted antibodies but impose more complex pharmacology, which hinders efforts to optimize the ligands prior to human applications. Human embryonic kidney 293T cells expressing the humanized single-chain variable fragment (scFv) C825 (huC825) with high-affinity for DOTA-haptens (293T-huC825) in a transmembrane-anchored format eliminated the requirement to use other pretargeting reagents and provided a simplified, accelerated assay of radiohapten capture while offering normalized cell surface expression of the molecular target of interest. Using binding assays, ex vivo biodistribution, and in vivo imaging, we demonstrated that radiohaptens based on benzyl-DOTA and a second generation “Proteus” DOTA-platform effectively and specifically engaged membrane-bound huC825, achieving favorable tumor-to-normal tissue uptake ratios in mice. Furthermore, [(86)Y]Y-DOTA-Bn predicted absorbed dose to critical organs with reasonable accuracy for both [(177)Lu]Lu-DOTA-Bn and [(225)Ac]Ac-Pr, which highlights the benefit of a dosimetry-based treatment approach.

Published

2021

15. Imaging of Cancer γ-Secretase Activity Using an Inhibitor-Based PET Probe

Author

George P. Liao, Thomas Li, Kelly E. Henry, Veronica L. Nagle, Blesida Punzalan, Xianzhong Wu, Jason S. Lewis, Lukas M. Carter, Naga Vara Kishore Pillarsetty, Pengju Nie, Teja Kalidindi, Georgia R. Frost, and Yue-Ming Li

Subjects

Cancer Research, Notch signaling pathway, Breast Neoplasms, Article, Iodine Radioisotopes, Mice, In vivo, medicine, Animals, Humans, Tissue Distribution, Mammary tumor, Receptors, Notch, Chemistry, Cancer, medicine.disease, In vitro, Oncology, Tumor progression, Positron-Emission Tomography, Cancer cell, Cancer research, Female, Amyloid Precursor Protein Secretases, Semagacestat, medicine.drug

Abstract

Purpose: Abnormal Notch signaling promotes cancer cell growth and tumor progression in various cancers. Targeting γ-secretase, a pivotal regulator in the Notch pathway, has yielded numerous γ-secretase inhibitors (GSIs) for clinical investigation in the last 2 decades. However, GSIs have demonstrated minimal success in clinical trials in part due to the lack of specific and precise tools to assess γ-secretase activity and its inhibition in vivo. Experimental Design: We designed an imaging probe based on GSI Semagacestat structure and synthesized the radioiodine-labeled analogues [131I]- or [124I]-PN67 from corresponding trimethyl-tin precursors. Both membrane- and cell-based ligand-binding assays were performed using [131I]-PN67 to determine the binding affinity and specificity for γ-secretase in vitro. Moreover, we evaluated [124I]-PN67 by PET imaging in mammary tumor and glioblastoma mouse models. Results: The probe was synthesized through iodo-destannylation using chloramine-T as an oxidant with a high labeling yield and efficiency. In vitro binding results demonstrate the high specificity of this probe and its ability for target replacement study by clinical GSIs. PET imaging studies demonstrated a significant (P < 0.05) increased in the uptake of [124I]-PN67 in tumors versus blocking or sham control groups across multiple mouse models, including 4T1 allograft, MMTV-PyMT breast cancer, and U87 glioblastoma allograft. Ex vivo biodistribution and autoradiography corroborate these results, indicating γ-secretase specific tumor accumulation of [124I]-PN67. Conclusions: [124I]-PN67 is a novel PET imaging agent that enables assessment of γ-secretase activity and target engagement of clinical GSIs.

Published

2021

16. 111In/225Ac theranostic pretargeting of nodular colorectal peritoneal carcinomatosis: preclinical SPECT and autoradiography studies

Author

Sebastian Chung, Christopher Chandler, Darren Veach, Michael McDevitt, Pat Zanzonico, Shin Seo, Blesida Punzalan, Daniela Burnes Vargas, Hong Xu, Hong-fen Guo, Ouathek Ouerfelli, Guangbin Yang, Andrea Cercek, Garrett Nash, Nai-Kong Cheung, Sarah Cheal, and Steven Larson

Subjects

Cancer Research, Molecular Medicine, Radiology, Nuclear Medicine and imaging

Published

2022

17. γ-Tocotrienol-Loaded Liposomes for Radioprotection from Hematopoietic Side Effects Caused by Radiotherapeutic Drugs

Author

Kishore Gangangari, Casey J. Lee, Soobin Park, Sang-gyu Lee, Michael G. Kharas, Steven M. Larson, Lisa Bodei, Hanzhi Lou, Blesida Punzalan, Naga Vara Kishore Pillarsetty, Teja Kalidindi, Hebert Alberto Vargas, Ariana Bitton, and Vijay K. Singh

Subjects

0301 basic medicine, medicine.medical_specialty, bone marrow, Population, Radiation-Protective Agents, Pharmacology, Flow cytometry, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Sinusoid, Internal medicine, medicine, Animals, Vitamin E, Radiology, Nuclear Medicine and imaging, Tissue Distribution, Chromans, Basic, education, gamma-Tocotrienol, education.field_of_study, EDTMP, Hematology, medicine.diagnostic_test, Radiotherapy, technology, industry, and agriculture, γ-tocotrienol, Hematopoiesis, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, chemistry, 030220 oncology & carcinogenesis, Liposomes, liposome, Bone marrow, radiation protection, Radiobiology/Dosimetry

Abstract

Visual Abstract, With the successful development and increased use of targeted radionuclide therapy for treating cancer comes the increased risk of radiation injury to bone marrow—both direct suppression and stochastic effects, leading to neoplasia. Herein, we report a novel radioprotector drug, a liposomal formulation of γ-tocotrienol (GT3), or GT3-Nano for short, to mitigate bone marrow radiation damage during targeted radionuclide therapy. Methods: GT3 was loaded into liposomes using passive loading. 64Cu-GT3-Nano and 3H-GT3-Nano were synthesized to study the in vivo biodistribution profile of the liposome and GT3 individually. The radioprotection efficacy of GT3-Nano was assessed after acute 137Cs whole-body irradiation at a sublethal (4 Gy), a lethal (9 Gy), or a single high-dose administration of 153Sm-ethylenediamine-N,N,N′,N′-tetrakis(methylene phosphonic acid) (EDTMP). Flow cytometry and fluorescence microscopy were used to analyze hematopoietic cell population dynamics and the cellular site of GT3-Nano localization in the spleen and bone marrow, respectively. Results: Bone marrow uptake and retention (percentage injected dose per gram of tissue) at 24 h was 6.98 ± 2.34 for 64Cu-GT3-Nano and 7.44 ± 2.52 for 3H-GT3-Nano. GT3-Nano administered 24 h before or after 4 Gy of total-body irradiation (TBI) promoted rapid and complete hematopoietic recovery, whereas recovery of controls stalled at 60%. GT3-Nano demonstrated dose-dependent radioprotection, achieving 90% survival at 50 mg/kg against lethal 9-Gy TBI. Flow cytometry of the bone marrow indicated that progenitor bone marrow cells MPP2 and CMP were upregulated in GT3-Nano–treated mice. Immunohistochemistry showed that GT3-Nano accumulates in CD105-positive sinusoid epithelial cells. Conclusion: GT3-Nano is highly effective in mitigating the marrow-suppressive effects of sublethal and lethal TBI in mice. GT3-Nano can facilitate rapid recovery of hematopoietic components in mice treated with the endoradiotherapeutic agent 153Sm-EDTMP.

Published

2020

18. ImmunoPET Imaging of Endogenous and Transfected Prolactin Receptor Tumor Xenografts

Author

Darren R. Veach, Valerie A. Longo, Blesida Punzalan, Jason T. Giurleo, Shutian Ruan, Amy Han, Jiong Wu, Steven M. Larson, Edward K. Fung, Jorge A. Carrasquillo, Sarah M. Cheal, Jessica R. Kirshner, Marcus Kelly, Pat Zanzonico, George Ehrlich, Gavin Thurston, and William C. Olson

Subjects

0301 basic medicine, Biodistribution, Immunoconjugates, Receptors, Prolactin, medicine.drug_class, Mice, Nude, Pharmaceutical Science, Monoclonal antibody, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Prostate, Cell Line, Tumor, Neoplasms, Drug Discovery, medicine, Animals, Humans, Tissue Distribution, IC50, biology, Chemistry, Prolactin receptor, Antibodies, Monoclonal, Transfection, Xenograft Model Antitumor Assays, In vitro, Molecular Imaging, 030104 developmental biology, medicine.anatomical_structure, Positron-Emission Tomography, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Molecular Medicine, Female, Radiopharmaceuticals, Antibody

Abstract

Antibodies labeled with positron-emitting isotopes have been used for tumor detection, predicting which patients may respond to tumor antigen-directed therapy, and assessing pharmacodynamic effects of drug interventions. Prolactin receptor (PRLR) is overexpressed in breast and prostate cancers and is a new target for cancer therapy. We evaluated REGN2878, an anti-PRLR monoclonal antibody, as an immunoPET reagent. REGN2878 was labeled with Zr-89 after conjugation with desferrioxamine B or labeled with I-131/ I-124. In vitro determination of the half-maximal inhibitory concentration (IC50) of parental REGN2878, DFO- REGN2878, and iodinated REGN2878 was performed by examining the effect of the increasing amounts of these on uptake of trace-labeled I-131 REGN2878. REGN1932, a non-PRLR binding antibody, was used as a control. Imaging and biodistribution studies were performed in mice bearing tumor xenografts with various expression levels of PRLR, including MCF-7, transfected MCF-7/PRLR, PC3, and transfected PC3/PRLR and T4D7v11 cell lines. The specificity of uptake in tumors was evaluated by comparing Zr-89 REGN2878 and REGN1932, and in vivo competition compared Zr-89 REGN2878 uptake in tumor xenografts with and without prior injection of 2 mg of nonradioactive REGN2878. The competition binding assay of DFO-REGN2878 at ratios of 3.53–5.77 DFO per antibody showed IC50 values of 0.4917 and 0.7136 nM, respectively, compared to 0.3455 nM for parental REGN2878 and 0.3343 nM for I-124 REGN2878. Imaging and biodistribution studies showed excellent targeting of Zr-89 REGN2878 in PRLR-positive xenografts at delayed times of 189 h (presented as mean ± 1 SD, percent injected activity per mL (%IA/mL) 74.6 ± 33.8%IA/mL). In contrast, MCF-7/PRLR tumor xenografts showed a low uptake (7.0 ± 2.3%IA/mL) of control Zr-89 REGN1932 and a very low uptake and rapid clearance of I-124 REGN2878 (1.4 ± 0.6%IA/mL). Zr-89 REGN2878 has excellent antigen-specific targeting in various PRLR tumor xenograft models. We estimated, using image-based kinetic modeling, that PRLR antigen has a very rapid in vivo turnover half-life of ~14 min from the cell membrane. Despite relatively modest estimated tumor PRLR expression numbers, PRLR-expressing cells have shown final retention of the Zr-89 REGN2878 antibody, with an uptake that appeared to be related to PRLR expression. This reagent has the potential to be used in clinical trials targeting PRLR.

Published

2018

19. Theranostic pretargeted radioimmunotherapy of internalizing solid tumor antigens in human tumor xenografts in mice: Curative treatment of HER2-positive breast carcinoma

Author

Hong-fen Guo, Pat Zanzonico, Sang-gyu Lee, Hong Xu, Blesida Punzalan, Meghan Bell, Edward K. Fung, Manisha Singh, Steven M. Larson, Sarah M. Cheal, Nai-Kong V. Cheung, Alessandra Piersigilli, Achim A. Jungbluth, and Mitesh Patel

Subjects

0301 basic medicine, Antibodies, Neoplasm, Receptor, ErbB-2, medicine.medical_treatment, pretargeting, Mice, Nude, Medicine (miscellaneous), Breast Neoplasms, Octreotide, Theranostic Nanomedicine, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigens, Neoplasm, Trastuzumab, HER2, Neuroblastoma, lutetium-177, Organometallic Compounds, Animals, Humans, Medicine, Pretargeted Radioimmunotherapy, Molecular Targeted Therapy, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), multistep targeting, business.industry, Cancer, Radioimmunotherapy, medicine.disease, 3. Good health, Disease Models, Animal, Regimen, Treatment Outcome, 030104 developmental biology, medicine.anatomical_structure, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, Heterografts, Bone marrow, bispecific antibodies, business, Neoplasm Transplantation, Research Paper, medicine.drug

Abstract

In recent reports, we have shown that optimized pretargeted radioimmunotherapy (PRIT) based on molecularly engineered antibody conjugates and 177Lu-DOTA chelate (DOTA-PRIT) can be used to cure mice bearing human solid tumor xenografts using antitumor antibodies to minimally internalizing membrane antigens, GPA33 (colon) and GD2 (neuroblastoma). However, many solid tumor membrane antigens are internalized after antibody binding and it is generally believed that internalizing tumor membrane antigens are not suitable targets for PRIT. In this study, we tested the hypothesis that DOTA-PRIT can be performed successfully to target HER2, an internalizing membrane antigen widely expressed in breast, ovarian, and gastroesophageal junction cancers. Methods: DOTA-PRIT was carried out in athymic nude mice bearing BT-474 xenografts, a HER2-expressing human breast cancer, using a three-step dosing regimen consisting of sequential intravenous administrations of: 1) a bispecific IgG-scFv (210 kD) format (BsAb) carrying the IgG sequence of the anti-HER2 antibody trastuzumab and the scFv “C825” with high-affinity, hapten-binding antibody for Bn-DOTA (metal) (BsAb: anti-HER2-C825), 2) a 500 kD dextran-based clearing agent, followed by 3) 177Lu-DOTA-Bn. At the time of treatment, athymic nude mice bearing established subcutaneous BT-474 tumors (medium- and smaller-sized tumors with tumor volumes of 209 ± 101 mm3 and ranging from palpable to 30 mm3, respectively), were studied along with controls. We studied single- and multi-dose regimens. For groups receiving fractionated treatment, we verified quantitative tumor targeting during each treatment cycle using non-invasive imaging with single-photon emission computed tomography/computed tomography (SPECT/CT). Results: We achieved high therapeutic indices (TI, the ratio of radiation-absorbed dose in tumor to radiation-absorbed dose to critical organs, such as bone marrow) for targeting in blood (TI = 28) and kidney (TI = 7), while delivering average radiation-absorbed doses of 39.9 cGy/MBq to tumor. Based on dosimetry estimates, we implemented a curative fractionated therapeutic regimen for medium-sized tumors that would deliver approximately 70 Gy to tumors, which required treatment with a total of 167 MBq 177Lu-DOTA-Bn/mouse (estimated absorbed tumor dose: 66 Gy). This regimen was well tolerated and achieved 100% complete responses (CRs; defined herein as tumor volume equal to or smaller than 4.2 mm3), including 62.5% histologic cure (5/8) and 37.5% microscopic residual disease (3/8) at 85 days (d). Treatment controls showed tumor progression to 207 ± 201% of pre-treatment volume at 85 d and no CRs. Finally, we show that treatment with this curative 177Lu regimen leads to a very low incidence of histopathologic abnormalities in critical organs such as bone marrow and kidney among survivors compared with non-treated controls. Conclusion: Contrary to popular belief, we demonstrate that DOTA-PRIT can be successfully adapted to an internalizing antigen-antibody system such as HER2, with sufficient TIs and absorbed tumor doses to achieve a high probability of cures of established human breast cancer xenografts while sparing critical organs of significant radiotoxicity.

Published

2018

20. Abstract P168: Pretargeted radioimmunotherapy using 225Ac for intraperitoneal Her2-expressing epithelial ovarian carcinoma xenografts

Author

Sebastian K. Chung, Christopher S. Chandler, Daniela Burnes Vargas, Shin H. Seo, Michael R. McDevitt, Darren Veach, Blesida Punzalan, Xu Hong, Hong-fen Guo, Garrett M. Nash, Andrea Cercek, Nai-Kong V. Cheung, Steven M. Larson, and Sarah M. Cheal

Subjects

Cancer Research, Oncology

Abstract

Objectives Epithelial ovarian carcinoma (EOC) is a common and lethal gynecologic malignancy that frequently presents as advanced staged disease, such as peritoneal carcinomatosis (PC). We previously reported cures in BT-474 murine xenografts with Pretargeted Radioimmunotherapy (PRIT) using 177Lu radiohaptens targeting Her2 via a bispecific antibody (BsAb). Here-in we report the use of PRIT with alpha emitter 225Ac labelled PrDOTA to treat a PC model of SKOV3, a Her2+ cell line of EOC. Methods 6 wk old female athymic nude mice inoculated IP with 1E5 luciferase/GFP-transfected SKOV3 cells were separated into 5 groups (n=10). Treatment mice received 1 or 2 cycles of Anti-Her2-C825 BsAb + [225Ac]PrDOTA (Her2-Targeted), at 14 and 21 days after inoculation, respectively. Control groups received Anti-Her2 BsAb only, Anti-GPA33 BsAb + [225Ac]PrDOTA (Off-Targeted) or no treatment. On cycle day 1, the mice were injected IP with 0.25mg (1.19nmol) BsAb. On cycle day 2, 25µg (2.76nmol) CCA16-DOTAY clearing agent (CA) was given IV 22h from BsAb. Mice in therapy groups were injected IP with 1µCi (0.74-0.79nmol) [225Ac]PrDOTA-Bn 4h after CA. Weekly weights and BLIs with IP cavity ROIs were obtained and normalized to the respective values for each mouse at week 0 pre-treatment. End points: weight loss >20% baseline, moribund, or severe abdominal distension. At 154 days, 15 surviving treatment and 1 untreated control mice were submitted for hematology and histopathology. Results Histologic cures and prolonged survival were demonstrated in treatment mice (17/20 at 133 days) as compared to control mice (12/27 at 133 d, Logrank p0.05; all weeks). BLI of mice treated with 1 and 2 cycle of Her2 PRIT decreased 47% when compared to baseline within 1 week (T test p=0.04), suggesting treatment effects as early as 1 week. There were no differences in weights when compared to baseline (2-way ANOVA p>0.05). While the untreated mouse had high peritoneal adenocarcinoma tumor burden, there was no histologic evidence of viable neoplasia in 15/15 submitted treatment mice. Treatment mice had moderate renal tubular degenerative lesions on histology, but this did not affect renal function based on serum BUN or Cr. All hematologic parameters were within normal limits for treated mice. Conclusions 1 and 2 cycles of [225Ac]PrDOTA-PRIT against Her2 resulted in histologic cures and prolonged survival in IP SKOV3 xenografts with minimal toxicity. The anti-Her2 PrDOTA-PRIT system is a promising theranostic approach for otherwise incurable PC. Citation Format: Sebastian K. Chung, Christopher S. Chandler, Daniela Burnes Vargas, Shin H. Seo, Michael R. McDevitt, Darren Veach, Blesida Punzalan, Xu Hong, Hong-fen Guo, Garrett M. Nash, Andrea Cercek, Nai-Kong V. Cheung, Steven M. Larson, Sarah M. Cheal. Pretargeted radioimmunotherapy using 225Ac for intraperitoneal Her2-expressing epithelial ovarian carcinoma xenografts [abstract]. In: Proceedings of the AACR-NCI-EORTC Virtual International Conference on Molecular Targets and Cancer Therapeutics; 2021 Oct 7-10. Philadelphia (PA): AACR; Mol Cancer Ther 2021;20(12 Suppl):Abstract nr P168.

Published

2021

21. Abstract 1391: Self-assembling and disassembling bispecific antibody platform for pretargeted radioimmunotherapy against GPA33 in a xenograft model of colorectal peritoneal carcinomatosis

Author

Darren Veach, Garrett M. Nash, Sebastian K. Chung, Hong-fen Guo, Blesida Punzalan, Christopher Chandler, Steven M. Larson, Shin Hyuk Seo, Brian H. Santich, Cheung Nai-Kong, Andrea Cercek, Mao Wang, Hong Xu, Sarah M. Cheal, and Daniela Burnes Vargas

Subjects

GPA33, Cancer Research, Bispecific antibody, Oncology, business.industry, Self assembling, Cancer research, Medicine, Pretargeted Radioimmunotherapy, business, Peritoneal carcinomatosis

Abstract

Objectives: There is increasing interest in the potential role of radioimmunotherapy in the treatment of peritoneal carcinomatosis (PC), locoregional metastasis throughout the peritoneal cavity. We recently described a SADA platform when applied to GD2-specific PRIT using beta and alpha emitting radioisotopes achieved exceptional therapeutic indices (TI) achieving tumor cures without myelo-, renal-, neuro-, or hepatic toxicities (1). We applied SADA technology to a tumor associated antigen GPA33 expressed by colorectal cancer in a PC model, and compared that to a 3 step PRIT which requires a clearing agent (CA), previously reported to produce durable responses including histologic cures of GPA33-expressing SW1222 subcutaneous (2) and intraperitoneal (ip) colorectal xenograft models (3). Methods: SADA BsAb built from a humanized anti-GPA33 single chain Fv (scFv) and a humanized anti-DOTA scFv were expressed using the Expi293 Expression System and purified by affinity chromatography (1). Biochemical purity of >90% was confirmed via size exclusion HPLC and antigen binding confirmed by surface plasmon resonance and by flow cytometry on GPA33(+) cell lines. 8 wk old female athymic nude mice were inoculated ip with 5E6 cells of stably luciferase/GFP-transfected SW1222 in 200 µL media. PC tumor progression was monitored by in vivo BLI. GPA33-SADA and control GD2-SADA were injected intravenously (iv) on day 26, followed 48 hr later with 1 mCi (37 MBq,200 pmol) [177Lu]Lu-DOTA-Bn ip. In the 3 step PRIT group, mice were treated with 250µg (1.19nmol) GPA33-BsAb (n=4) followed 24 hr later by 20 µg (2.21 nmol) of CA iv, before the injection of 1 mCi (37 MBq,200 pmol) [177Lu]Lu-DOTA-Bn ip 4 hr later. In an additional control group, no SADA was given before 1 mCi (37 MBq,200 pmol) [177Lu]Lu-DOTA-Bn ip. Biodistribution was performed 24 hr after injection of ip 177Lu radiohapten. Results: Radioactivity absorbed in harvested ip SW1222 xenograft tumors treated with SADA-GPA33 (4.92 + 1.59 [mean + SD] percentage injected dose per gram [%ID/g]) was greater than that of harvested tumors treated with the traditional 3 step PRIT to GPA33 (2.68 + 0.179 %ID/g, p=0.043) or with negative control SADA-GD2 (0.513 + 0.293 %ID/g, p Conclusions: SADA-PRIT targeting GPA33 has favorable TI for colorectal PC. When compared to 3 step PRIT, SADA showed more selectivity and TI. {{References}}: 1. Santich BH, Cheal SM, Ahmed M, et al. Clin Cancer Res. 2020; 2. Cheal SM, Xu H, Guo HF, et al. Eur J Nucl Med Mol Imaging. 2016;43(5):925-937.3. Chandler C, Cheal SM, Nash G, et al. Journal of Nuclear Medicine. 2020;61. Citation Format: Sebastian Chung, Mao Wang, Darren Veach, Sarah Cheal, Daniela Burnes Vargas, Shin Hyuk Seo, Blesida Punzalan, Brian Santich, Hong-fen Guo, Hong Xu, Garrett Nash, Andrea Cercek, Christopher Chandler, Steven Larson, Nai-Kong Cheung. Self-assembling and disassembling bispecific antibody platform for pretargeted radioimmunotherapy against GPA33 in a xenograft model of colorectal peritoneal carcinomatosis [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1391.

Published

2021

22. Repeatability of [68Ga]DKFZ11-PSMA PET Scans for Detecting Prostate-specific Membrane Antigen-positive Prostate Cancer

Author

Daniel E. Spratt, Kishore Gangangari, Joseph R. Osborne, Blesida Punzalan, Steven M. Larson, Naga Vara Kishore Pillarsetty, Teja Kalidindi, and Wolfgang A. Weber

Subjects

Male, Cancer Research, Biodistribution, Gallium Radioisotopes, urologic and male genital diseases, Article, 030218 nuclear medicine & medical imaging, Lesion, Mice, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Region of interest, Cell Line, Tumor, Glutamate carboxypeptidase II, medicine, Animals, Humans, Tissue Distribution, Radiology, Nuclear Medicine and imaging, medicine.diagnostic_test, Chemistry, business.industry, Prostatic Neoplasms, Reproducibility of Results, Repeatability, Prostate-Specific Antigen, medicine.disease, Xenograft Model Antitumor Assays, Oncology, Positron emission tomography, Positron-Emission Tomography, 030220 oncology & carcinogenesis, Psma pet, Radiopharmaceuticals, medicine.symptom, Nuclear medicine, business

Abstract

We studied the effect of varying specific activity of [68Ga]DKFZ-PSMA11 ([68Ga]DP11) on repeated imaging of prostate-specific membrane antigen-positive (PSMA+) xenograft tumors. Athymic nude mice bearing PC3-PIP (PSMA+) and PC3 (PSMA−) bilateral flank tumors were assessed to study intra- and inter-day repeatability of [68Ga]DP11 imaging in mice administered [68Ga]DP11 or [67Ga]DP11 (as a dilution tracer) using imaging and biodistribution studies. Region of interest (ROI) analysis of the [68Ga]DP11 imaging study indicated that the uptake was constant on the same day or consecutive days. Prior imaging with [68Ga]DP11 did not significantly influence the subsequent uptake of [68Ga]DP11. Uptake of [68Ga]DP11 (60 min) and [67Ga]DP11 (24 h) in PC3-PIP tumors was 12.37 ± 4.19 %ID/g and 12.49 ± 6.88 %ID/g, respectively; [68Ga]DP11 was 13.83 ± 3.77 and 17.76 ± 1.84 on same-day and 15.98 ± 5.82 %ID/g on second-day imaging. This study demonstrates that [68Ga]DP11, in a given PSMA+ lesion, is constant under several same-day or serial-day imaging conditions.

Published

2017

23. Paradigms for Precision Medicine in Epichaperome Cancer Therapy

Author

Blesida Punzalan, Monica L. Guzman, Gabriela Chiosis, Nagavarakishore Pillarsetty, Nicolas Lecomte, Thomas Ku, Connie W. Batlevi, Jason S. Lewis, Mary L. Alpaugh, Larry Norton, Alexander Bolaender, Jacek Koziorowski, Anas Younes, Eva Burnazi, Komal Jhaveri, Anna Rodina, Mohammad M. Uddin, Gail J. Roboz, Suhasini Joshi, Smit K. Shah, Tai Wang, Mark Dunphy, Anson Ku, Pengrong Yan, Pat Zanzonico, Adriana D. Corben, Yelena Y. Janjigian, Shanu Modi, Tony Taldone, Eloisi Caldas-Lopes, Steven M. Larson, Serge K. Lyashchenko, and John F. Gerecitano

Subjects

0301 basic medicine, Cancer Research, Proteome, Computer science, Cancer therapy, Antineoplastic Agents, Computational biology, Article, Drug Administration Schedule, Theranostic Nanomedicine, Malignant transformation, Epigenesis, Genetic, 03 medical and health sciences, Mice, 0302 clinical medicine, Interaction network, Cell Line, Tumor, Neoplasms, Protein Interaction Mapping, medicine, Animals, Humans, HSP90 Heat-Shock Proteins, Protein Interaction Maps, Precision Medicine, Dose-Response Relationship, Drug, Cancer, Cell Biology, medicine.disease, Precision medicine, Xenograft Model Antitumor Assays, Pharmacometrics, Biomarker (cell), Molecular Imaging, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Female, Protein network, Biomarkers, Molecular Chaperones

Abstract

Alterations in protein-protein interaction networks are at the core of malignant transformation but have yet to be translated into appropriate diagnostic tools. We make use of the kinetic selectivity properties of an imaging probe to visualize and measure the epichaperome, a pathologic protein-protein interaction network. We are able to assay and image epichaperome networks in cancer and their engagement by inhibitor in patients’ tumors at single-lesion resolution in real time, and demonstrate that quantitative evaluation at the level of individual tumors can be used to optimize dose and schedule selection. We thus provide preclinical and clinical evidence in the use of this theranostic platform for precision-medicine targeting of the aberrant properties of protein networks.

Published

2019

24. Copper-64 labeled liposomes for imaging bone marrow

Author

Naga Vara Kishore Pillarsetty, Teja Kalidindi, Blesida Punzalan, Sang-gyu Lee, Steven M. Larson, and Kishore Gangangari

Subjects

Male, Cancer Research, Biodistribution, Pathology, medicine.medical_specialty, Stromal cell, Drug Compounding, Mice, Nude, 02 engineering and technology, Article, 030218 nuclear medicine & medical imaging, Mice, 03 medical and health sciences, 0302 clinical medicine, Bone Marrow, Positron Emission Tomography Computed Tomography, medicine, Animals, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Liposome, medicine.diagnostic_test, Chemistry, Soft tissue, 021001 nanoscience & nanotechnology, Haematopoiesis, medicine.anatomical_structure, Copper Radioisotopes, Positron emission tomography, Isotope Labeling, Liposomes, Cancer research, Molecular Medicine, Bone marrow, Stem cell, 0210 nano-technology

Abstract

Introduction Bone marrow is the soft tissue compartment inside the bones made up of hematopoietic cells, adipocytes, stromal cells, phagocytic cells, stem cells, and sinusoids. While [ 18 F]-FLT has been utilized to image proliferative marrow, to date, there are no reports of particle based positron emission tomography (PET) imaging agents for imaging bone marrow. We have developed copper-64 labeled liposomal formulation that selectively targets bone marrow and therefore serves as an efficient PET probe for imaging bone marrow. Methods Optimized liposomal formulations were prepared with succinyl PE, DSPC, cholesterol, and mPEG-DSPE (69:39:1:10:0.1) with diameters of 90 and 140nm, and were doped with DOTA-Bn-DSPE for stable 64 Cu incorporation into liposomes. Results PET imaging and biodistribution studies with 64 Cu-labeled liposomes indicate that accumulation in bone marrow was as high as 15.18±3.69%ID/g for 90nm liposomes and 7.01±0.92%ID/g for 140nm liposomes at 24h post-administration. In vivo biodistribution studies in tumor-bearing mice indicate that the uptake of 90nm particles is approximately 0.89±0.48%ID/g in tumor and 14.22±8.07%ID/g in bone marrow, but respective values for Doxil® like liposomes are 0.83±0.49%ID/g and 2.23±1.00%ID/g. Conclusion Our results indicate that our novel PET labeled liposomes target bone marrow with very high efficiency and therefore can function as efficient bone marrow imaging agents.

Published

2016

25. Theranostic pretargeted radioimmunotherapy of colorectal cancer xenografts in mice using picomolar affinity 86Y- or 177Lu-DOTA-Bn binding scFv C825/GPA33 IgG bispecific immunoconjugates

Author

Jorge A. Carrasquillo, Joseph A. O'Donoghue, Sandhya Chalasani, Pat Zanzonico, K. Dane Wittrup, Achim A. Jungbluth, Peter Smith-Jones, Hong Xu, Blesida Punzalan, Sang-gyu Lee, Edward K. Fung, Hong-fen Guo, Nai-Kong V. Cheung, Steven M. Larson, and Sarah M. Cheal

Subjects

0301 basic medicine, Colorectal cancer, business.industry, medicine.medical_treatment, General Medicine, medicine.disease, Tumor antigen, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Antigen, In vivo, 030220 oncology & carcinogenesis, Radioimmunotherapy, Immunology, Cancer research, medicine, DOTA, Radiology, Nuclear Medicine and imaging, Pretargeted Radioimmunotherapy, business, Pretargeting

Abstract

GPA33 is a colorectal cancer (CRC) antigen with unique retention properties after huA33-mediated tumor targeting. We tested a pretargeted radioimmunotherapy (PRIT) approach for CRC using a tetravalent bispecific antibody with dual specificity for GPA33 tumor antigen and DOTA-Bn–(radiolanthanide metal) complex. PRIT was optimized in vivo by titrating sequential intravenous doses of huA33-C825, the dextran-based clearing agent, and the C825 haptens 177Lu-or 86Y-DOTA-Bn in mice bearing the SW1222 subcutaneous (s.c.) CRC xenograft model. Using optimized PRIT, therapeutic indices (TIs) for tumor radiation-absorbed dose of 73 (tumor/blood) and 12 (tumor/kidney) were achieved. Estimated absorbed doses (cGy/MBq) to tumor, blood, liver, spleen, and kidney for single-cycle PRIT were 65.8, 0.9 (TI 73), 6.3 (TI 10), 6.6 (TI 10), and 5.3 (TI 12), respectively. Two cycles of PRIT (66.6 or 111 MBq 177Lu-DOTA-Bn) were safe and effective, with a complete response of established s.c. tumors (100 – 700 mm3) in nine of nine mice, with two mice alive without recurrence at >140 days. Tumor log kill in this model was estimated to be 2.1 – 3.0 based on time to 500-mm3 tumor recurrence. In addition, PRIT dosimetry/diagnosis was performed by PET imaging of the positron-emitting DOTA hapten 86Y-DOTA-Bn. We have developed anti-GPA33 PRIT as a triple-step theranostic strategy for preclinical detection, dosimetry, and safe targeted radiotherapy of established human colorectal mouse xenografts.

Published

2015

26. Evaluation of Glycodendron and Synthetically Modified Dextran Clearing Agents for Multistep Targeting of Radioisotopes for Molecular Imaging and Radioimmunotherapy

Author

Don B. Axworthy, Anna Dilhas, Pat Zanzonico, Sarah M. Cheal, Steven M. Larson, Ouathek Ouerfelli, Geralda Torchon, Guangbin Yang, Jun Pu, Barney Yoo, Blesida Punzalan, and Sarah Boughdad

Subjects

Streptavidin, medicine.medical_treatment, Pharmaceutical Science, Article, Mice, chemistry.chemical_compound, Drug Delivery Systems, Drug Stability, Biotin, Coordination Complexes, In vivo, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Pretargeting, Radioisotopes, Molecular Structure, Chemistry, Dextrans, Radioimmunotherapy, Fusion protein, Molecular Imaging, Dextran, Carbohydrate Sequence, Biochemistry, Positron-Emission Tomography, Colonic Neoplasms, Heterografts, Molecular Medicine, Molecular imaging

Abstract

A series of N-acetylgalactosamine-dendrons (NAG-dendrons) and dextrans bearing biotin moieties were compared for their ability to complex with and sequester circulating bispecific anti-tumor antibody (scFv4) streptavidin (SA) fusion protein (scFv4-SA) in vivo, to improve tumor to normal tissue concentration ratios for targeted radioimmunotherapy and diagnosis. Specifically, a total of five NAG-dendrons employing a common synthetic scaffold structure containing 4, 8, 16, or 32 carbohydrate residues and a single biotin moiety were prepared (NAGB), and for comparative purposes, a biotinylated-dextran with average molecular weight (MW) of 500 kD was synthesized from amino-dextran (DEXB). One of the NAGB compounds, CA16, has been investigated in humans; our aim was to determine if other NAGB analogs (e.g. CA8 or CA4) were bioequivalent to CA16 and/or better suited as MST reagents. In vivo studies included dynamic positron-emission tomography (PET) imaging of 124I-labelled-scFv4-SA clearance and dual-label biodistribution studies following multi-step targeting (MST) directed at subcutaneous (s.c.) human colon adenocarcinoma xenografts in mice. The MST protocol consists of three injections: first, a bispecific antibody specific for an anti-tumor associated glycoprotein (TAG-72) single chain genetically-fused with SA (scFv4-SA); second, CA16 or other clearing agent; and third, radiolabeled biotin. We observed using PET imaging of 124I-labelled-scFv4-SA clearance that the spatial arrangement of ligands conjugated to NAG (i.e. biotin) can impact the binding to antibody in circulation and subsequent liver uptake of the NAG-antibody complex. Also, NAGB CA32-LC or CA16-LC can be utilized during MST to achieve comparable tumor- to-blood ratios and absolute tumor uptake seen previously with CA16. Finally, DEXB was equally effective as NAGB CA32-LC at lowering scFv4-SA in circulation, but at the expense of reducing absolute tumor uptake of radiolabeled biotin.

Published

2013

27. In Vivo Imaging of Bcr-Abl Overexpressing Tumors with a Radiolabeled Imatinib Analog as an Imaging Surrogate for Imatinib

Author

Blesida Punzalan, Athanasios Glekas, Nagavarakishore Pillarsetty, Peter Smith-Jones, Steven M. Larson, and Nahida Khan

Subjects

Models, Molecular, Biodistribution, Time Factors, medicine.drug_class, Fusion Proteins, bcr-abl, Pharmacology, Crystallography, X-Ray, Article, Piperazines, Tyrosine-kinase inhibitor, Mice, In vivo, Catalytic Domain, Cell Line, Tumor, hemic and lymphatic diseases, Animals, Humans, Medicine, Radiology, Nuclear Medicine and imaging, neoplasms, ABL, Dose-Response Relationship, Drug, business.industry, Imatinib, Imaging agent, Pyrimidines, Imatinib mesylate, Models, Chemical, Benzamides, Imatinib Mesylate, K562 Cells, business, Tyrosine kinase, Neoplasm Transplantation, Protein Binding, medicine.drug

Abstract

Imatinib mesylate is a tyrosine kinase inhibitor that was approved by the U.S. Food and Drug Administration in 2001 for treatment of many different stages of chronic myeloid leukemia and in 2002 for treatment of gastrointestinal stromal tumors. Imatinib is known to inhibit the dysregulated proliferation of chronic myeloid leukemia, which is associated with the Bcr-Abl kinase; in gastrointestinal stromal tumors, imatinib is known to act via c-Kit kinase inhibition. The objective of this study was to synthesize an 18F-labeled analog of imatinib not as a primary imaging agent but rather as a tracer for in vivo drug distribution and tracer concentration that can be used as a PET imaging surrogate for imatinib. Methods: Molecular modeling studies based on the crystal structure of imatinib bound to the active site of Abl were performed for designing the fluorinated analog. A 2-fluoroethyl analog of imatinib (SKI696) was synthesized using well-established procedures. The selectivity and binding affinity of SKI696 were compared with those of imatinib in vitro. Mice bearing K562 tumor xenografts, which are known to overexpress Bcr-Abl, were imaged with 18F-SKI696 PET. A biodistribution study was also performed on K562 tumor–bearing mice to which our radiolabeled tracer was administered. Results: The kinase assay verified that imatinib and SKI696 bind to the same targets with similar affinities. The feasibility of using 18F-SKI696 as a PET agent was examined in vivo, and 18F-SKI696 PET was shown to visualize K562 tumor xenografts in nude mice. The tumor was visible on PET 1 h after injection, with uptake of 1% of the injected dose. Biodistribution studies in K562-bearing mice were also performed, and the uptake of 18F-SKI696 (percentage injected dose per gram) for each organ was calculated. Conclusion: The results of the binding assay showed that SKI696 has selectivity and binding affinity comparable to imatinib. Small-animal PET of K562 tumor–bearing mice using 18F-SKI696 as a PET agent displayed promising tumor uptake and tumor-to-nontarget contrast. Because 18F-SKI696 has been taken up in vivo by tumors that overexpress Bcr-Abl, we are exploring a possible role for identifying tumors that will respond to imatinib before therapy.

Published

2011

28. Optimizing tumor targeting of the lipophilic EGFR-binding radiotracer SKI 243 using a liposomal nanoparticle delivery system

Author

Steven M. Larson, Valerie A. Longo, Pat Zanzonico, Nagavarakishore Pillarsetty, Peter Smith-Jones, Blesida Punzalan, Mithat Gonen, Athanasios Glekas, and Oula Penate Medina

Subjects

medicine.medical_specialty, animal structures, Mice, Nude, Pharmaceutical Science, Antineoplastic Agents, Article, Mice, Pharmacokinetics, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Epidermal growth factor receptor, EGFR inhibitors, Liposome, biology, business.industry, Cancer, medicine.disease, Surgery, ErbB Receptors, Positron-Emission Tomography, Liposomes, Drug delivery, Lipophilicity, Cancer research, biology.protein, Radiopharmaceuticals, Drug carrier, business, human activities

Abstract

Positron emission tomography (PET) of epidermal growth factor receptor (EGFR) kinase-specific radiolabeled tracers could provide a means for non-invasively characterizing EGFR expression and signaling activity in patients' tumors before, during, and after therapy with EGFR inhibitors. Towards this goal, our group has developed PET tracers which irreversibly bind to EGFR. However, tumor uptake is relatively low because of both the lipophilicity of such tracers (e.g. the morpholino-[124I]-IPQA [SKI 212243]), with octanol-to-water partition coefficients of up to 4, and a short dwell time in the blood and significant hepatobiliary clearance and intestinal reuptake. Liposomal nanoparticle delivery systems may favorably alter the pharmacokinetic profile and improve tumor targeting of highly lipophilic but otherwise promising cancer imaging tracers, such as the EGFR inhibitor SKI 243. SKI 243 is therefore an interesting model molecule for incorporation into lipid-based nanoparticles, as it would not only improve their solubility but also increase the circulation time, availability and, potentially, targeting of tumors. In the current study, we compared the pharmacokinetics and tumor targeting of the bare EGFR kinase-targeting radiotracer SKI 212243 (SKI 243) with that of the same tracer embedded in liposomes. SKI 243 and liposomal SKI 243 are both taken up by tumor xenografts but liposomal SKI 243 remained in the blood longer and consequently exhibited a 3- to 6-fold increase in uptake in the tumor among several other organs.

Published

2011

29. 2-18F-Fluoropropionic Acid as a PET Imaging Agent for Prostate Cancer

Author

Naga Vara Kishore Pillarsetty, Steven M. Larson, and Blesida Punzalan

Subjects

Male, Octanols, Biodistribution, Acetates, Article, 2-18F-fluoropropionic acid, Mice, Prostate cancer, Prostate, LNCaP, medicine, Animals, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Carbon Radioisotopes, Radioactive Tracers, Fluorocarbons, medicine.diagnostic_test, business.industry, Chemistry, Prostatic Neoplasms, Water, Tail vein, Pet imaging, medicine.disease, medicine.anatomical_structure, Positron emission tomography, Positron-Emission Tomography, Propionates, Nuclear medicine, business

Abstract

There is a high interest in developing an (18)F-labeled PET tracer that can aid in diagnosis and therapy monitoring of prostate cancer. In the current study, we have evaluated the potential of 2-(18)F-fluoropropionic acid ((18)F-FPA) as a PET tracer for imaging prostate cancer.(18)F-FPA was synthesized starting from methyl-2-bromopropionate. Small-animal PET studies were performed on mice with CWR22rv1, PC-3, DU-145, and LNCaP prostate xenografts, and comparison of imaging characteristics of (18)F-FPA with (18)F-FDG uptake is reported. Biodistribution studies with (18)F-FPA were performed on mice with CWR22rv1 xenografts and compared with (14)C-acetate.(18)F-FPA was synthesized in 44% overall radiochemical yield (decay-corrected). Small-animal PET studies revealed that (18)F-FPA can delineate both androgen-dependent and androgen-independent prostate xenografts with high tumor-to-background ratios. Comparative imaging studies demonstrate the superior performance of (18)F-FPA over (18)F-FDG for imaging prostate cancer, with excellent tumor-to-background contrast. Biodistribution studies show that tumor uptake of the tracer was 5.52 +/- 0.35, 5.53 +/- 0.42, 5.74 +/- 0.54, and 5.34 +/- 0.19 percentage injected dose (%ID) per gram at 1, 2, 3, and 4 h, respectively, after injection. The %ID/g values for (18)F-FPA and (14)C-acetate 1 h after tail vein injection were 7.08 +/- 0.80 and 0.36 +/- 0.08 in tumor, and the corresponding tumor-to-muscle ratios were 1.94 and 2.06, respectively.The data presented here indicate that (18)F-FPA accumulates in prostate cancers with high tumor-to-background ratios. (18)F-FPA has potential for use in the clinical diagnosis of prostate cancer in humans.

Published

2009

30. Sensitive in vivo imaging of T cells using a membrane-bound Gaussia princeps luciferase

Author

James Lee, Blesserene Punzalan, Steven M. Larson, Blesida Punzalan, Yan Nikhamin, Raymond Yeh, Michel Sadelain, Elmer Santos, Renier J. Brentjens, and Krista M.D. La Perle

Subjects

biology, medicine.diagnostic_test, T cell, General Medicine, Gaussia princeps, biology.organism_classification, Molecular biology, General Biochemistry, Genetics and Molecular Biology, Chimeric antigen receptor, Flow cytometry, Gaussia, medicine.anatomical_structure, In vivo, medicine, Bioluminescence, Luciferase

Abstract

We developed a new approach to bioluminescent T cell imaging using a membrane-anchored form of the Gaussia luciferase (GLuc) enzyme, termed extGLuc, which we could stably express in both mouse and human primary T cells. In vitro, extGLuc+ cells emitted significantly higher bioluminescent signal when compared to cells expressing GLuc, Renilla luciferase (RLuc) or membrane-anchored RLuc (extRLuc). In vivo, mouse extGLuc+ T cells showed higher bioluminescent signal when compared to GLuc+ and RLuc+ T cells. Application of this imaging approach to human T cells genetically modified to express tumor-specific chimeric antigen receptors (CARs) enabled us to show in vivo CAR-mediated T cell accumulation in tumor, T cell persistence over time and concomitant imaging of T cells and tumor cells modified to express firefly luciferase. This sensitive imaging technology has application to many in vivo cell-based studies in a wide array of mouse models.

Published

2009

31. Theranostic pretargeted radioimmunotherapy of colorectal cancer xenografts in mice using picomolar affinity ⁸⁶Y- or ¹⁷⁷Lu-DOTA-Bn binding scFv C825/GPA33 IgG bispecific immunoconjugates

Author

Sarah M, Cheal, Hong, Xu, Hong-Fen, Guo, Sang-Gyu, Lee, Blesida, Punzalan, Sandhya, Chalasani, Edward K, Fung, Achim, Jungbluth, Pat B, Zanzonico, Jorge A, Carrasquillo, Joseph, O'Donoghue, Peter M, Smith-Jones, K Dane, Wittrup, Nai-Kong V, Cheung, and Steven M, Larson

Subjects

Immunoconjugates, Membrane Glycoproteins, Antibody Affinity, Lutetium, Radioimmunotherapy, Xenograft Model Antitumor Assays, Article, Mice, Immunoglobulin G, Antibodies, Bispecific, Animals, Yttrium Radioisotopes, Radiopharmaceuticals, Colorectal Neoplasms, Single-Chain Antibodies

Abstract

GPA33 is a colorectal cancer (CRC) antigen with unique retention properties after huA33-mediated tumor targeting. We tested a pretargeted radioimmunotherapy (PRIT) approach for CRC using a tetravalent bispecific antibody with dual specificity for GPA33 tumor antigen and DOTA-Bn-(radiolanthanide metal) complex.PRIT was optimized in vivo by titrating sequential intravenous doses of huA33-C825, the dextran-based clearing agent, and the C825 haptens (177)Lu-or (86)Y-DOTA-Bn in mice bearing the SW1222 subcutaneous (s.c.) CRC xenograft model.Using optimized PRIT, therapeutic indices (TIs) for tumor radiation-absorbed dose of 73 (tumor/blood) and 12 (tumor/kidney) were achieved. Estimated absorbed doses (cGy/MBq) to tumor, blood, liver, spleen, and kidney for single-cycle PRIT were 65.8, 0.9 (TI 73), 6.3 (TI 10), 6.6 (TI 10), and 5.3 (TI 12), respectively. Two cycles of PRIT (66.6 or 111 MBq (177)Lu-DOTA-Bn) were safe and effective, with a complete response of established s.c. tumors (100 - 700 mm(3)) in nine of nine mice, with two mice alive without recurrence at140 days. Tumor log kill in this model was estimated to be 2.1 - 3.0 based on time to 500-mm(3) tumor recurrence. In addition, PRIT dosimetry/diagnosis was performed by PET imaging of the positron-emitting DOTA hapten (86)Y-DOTA-Bn.We have developed anti-GPA33 PRIT as a triple-step theranostic strategy for preclinical detection, dosimetry, and safe targeted radiotherapy of established human colorectal mouse xenografts.

Published

2015

32. Erratum to: Repeatability of [68Ga]DKFZ11-PSMA PET Scans for Detecting Prostate-specific Membrane Antigen-positive Prostate Cancer

Author

Blesida Punzalan, Kishore Gangangari, Wolfgang A. Weber, Naga Vara Kishore Pillarsetty, Joseph R. Osborne, Daniel E. Spratt, Teja Kalidindi, and Steven M. Larson

Subjects

Cancer Research, Prostate cancer, Oncology, Psma pet, Glutamate carboxypeptidase II, Cancer research, medicine, Radiology, Nuclear Medicine and imaging, Repeatability, Molecular imaging, medicine.disease

Published

2017

33. N-Acetylgalactosamino Dendrons as Clearing Agents to Enhance Liver Targeting of Model Antibody-Fusion Protein

Author

Jun Pu, Blesida Punzalan, Geralda Torchon, Guangbin Yang, Steven M. Larson, Anna Dilhas, Barney Yoo, Ouathek Ouerfelli, and Sarah M. Cheal

Subjects

Streptavidin, Biodistribution, Dendrimers, Acetylgalactosamine, medicine.medical_treatment, Recombinant Fusion Proteins, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Article, Iodine Radioisotopes, chemistry.chemical_compound, Mice, Dendrimer, medicine, Single-chain variable fragment, Animals, Clearing Agent, Pharmacology, Organic Chemistry, Fusion protein, Dextran, chemistry, Biochemistry, Liver, Radioimmunotherapy, Female, Biotechnology, Single-Chain Antibodies

Abstract

Dendrimer clearing agents represent a unique class of compounds for use in multistep targeting (MST) in radioimmunotherapy and imaging. These compounds were developed to facilitate the removal of excess tumor-targeting monoclonal antibody (mAb) prior to administration of the radionuclide to minimize exposure of normal tissue to radiation. Clearing agents are designed to capture the circulating mAb, and target it to the liver for metabolism. Glycodendrons are ideally suited for MST applications as these highly branched compounds are chemically well-defined, thus advantageous over heterogeneous macromolecules. Previous studies have described glycodendron 3 as a clearing agent for use in three-step MST protocols, and early in vivo assessment of 3 showed promise. However, synthetic challenges have hampered its availability for further development. In this report we describe a new sequence of chemical steps which enables the straightforward synthesis and analytical characterization of this class of dendrons. With accessibility and analytical identification solved, we sought to evaluate both lower and higher generation dendrons for hepatocyte targeting as well as clearance of a model protein. We prepared a series of clearing agents where a single biotin is connected to glycodendrons displaying four, eight, sixteen or thirty-two α-thio-N-acetylgalactosamine (α-SGalNAc) units, resulting in compounds with molecular weights ranging from 2 to 17 kDa, respectively. These compounds were fully characterized by LCMS and NMR. We then evaluated the capacity of these agents to clear a model (131)I-labeled single chain variable fragment antibody-streptavidin ((131)I-scFv-SAv) fusion protein from blood and tissue in mice, and compared their clearing efficiencies to that of a 500 kDa dextran-biotin conjugate. Glycodendrons and dextran-biotin exhibited enhanced blood clearance of the scFv-SAv construct. Biodistribution analysis showed liver targeting/uptake of the scFv-SAv construct to be 2-fold higher for compounds 1 to 4, as well as for the 500 kDa dextran, over saline. Additionally, the data suggest the glycodendrons clear through the liver, whereas the dextran through reticuloendothelial system (RES) metabolism.

Published

2013

34. Pairwise comparison of 89Zr- and 124I-labeled cG250 based on positron emission tomography imaging and nonlinear immunokinetic modeling: in vivo carbonic anhydrase IX receptor binding and internalization in mouse xenografts of clear-cell renal cell carcinoma

Author

Sarah M. Cheal, Michael J. Evans, Steven M. Larson, Jason S. Lewis, Blesida Punzalan, Michael G. Doran, Pat Zanzonico, and Joseph R. Osborne

Subjects

Pathology, Iodine Radioisotopes, Mice, Renal cell carcinoma, Monoclonal, Tissue Distribution, Internalization, Cancer, media_common, Carbonic Anhydrases, Tumor, medicine.diagnostic_test, biology, Chemistry, Antibodies, Monoclonal, General Medicine, Other Physical Sciences, Nuclear Medicine & Medical Imaging, Positron emission tomography, Biomedical Imaging, Antibody, Protein Binding, medicine.medical_specialty, media_common.quotation_subject, Clinical Sciences, Bioengineering, Antibodies, Article, Cell Line, Rare Diseases, In vivo, Antigens, Neoplasm, Cell Line, Tumor, medicine, Carcinoma, Animals, Humans, Radiology, Nuclear Medicine and imaging, Antigens, Carbonic Anhydrase IX, Carcinoma, Renal Cell, Renal Cell, medicine.disease, Xenograft Model Antitumor Assays, Clear cell renal cell carcinoma, Kinetics, Cell culture, Positron-Emission Tomography, Cancer research, biology.protein, Neoplasm, Zirconium

Abstract

PurposeThe PET tracer, (124)I-cG250, directed against carbonic anhydrase IX (CAIX) shows promise for presurgical diagnosis of clear-cell renal cell carcinoma (ccRCC) (Divgi et al. in Lancet Oncol 8:304-310, 2007; Divgi et al. in J Clin Oncol 31:187-194, 2013). The radiometal (89)Zr, however, may offer advantages as a surrogate PET nuclide over (124)I in terms of greater tumor uptake and retention (Rice et al. in Semin Nucl Med 41:265-282, 2011). We have developed a nonlinear immunokinetic model to facilitate a quantitative comparison of absolute uptake and antibody turnover between (124)I-cG250 and (89)Zr-cG250 using a human ccRCC xenograft tumor model in mice. We believe that this unique model better relates quantitative imaging data to the salient biological features of tumor antibody-antigen binding and turnover.MethodsWe conducted experiments with (89)Zr-cG250 and (124)I-cG250 using a human ccRCC cell line (SK-RC-38) to characterize the binding affinity and internalization kinetics of the two tracers in vitro. Serial PET imaging was performed in mice bearing subcutaneous ccRCC tumors to simultaneously detect and quantify time-dependent tumor uptake in vivo. Using the known specific activities of the two tracers, the equilibrium rates of antibody internalization and turnover in the tumors were derived from the PET images using nonlinear compartmental modeling.ResultsThe two tracers demonstrated virtually identical tumor cell binding and internalization but showed markedly different retentions in vitro. Superior PET images were obtained using (89)Zr-cG250, owing to the more prolonged trapping of the radiolabel in the tumor and simultaneous washout from normal tissues. Estimates of cG250/CAIX complex turnover were 1.35 - 5.51 × 10(12) molecules per hour per gram of tumor (20 % of receptors internalized per hour), and the ratio of (124)I/(89)Zr atoms released per unit time by tumor was 17.5.ConclusionPairwise evaluation of (89)Zr-cG250 and (124)I-cG250 provided the basis for a nonlinear immunokinetic model which yielded quantitative information about the binding and internalization of radioantibody bound to CAIX on tumor cells in vivo. (89)Zr-cG250 is likely to provide high-quality PET images and may be a useful tool to quantify CAIX/cG250 receptor turnover and cG250-accessible antigen density noninvasively in humans.

Published

2013

35. Abstract 5202: Comparison of [124I]-FIAC and [18F]-FAC as potential biomarkers to predict response to gemcitabine therapy in pancreatic cancers

Author

Brendan Huang, Nagavarakishore Pillarsetty, Kishore K. Gangangari, and Blesida Punzalan

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Potential biomarkers, Internal medicine, medicine, business, Gemcitabine, medicine.drug

Abstract

Pancreatic cancer (PaCa) is one of the most lethal kinds of cancers because it is virtually symptom free in early stages, metastasizes rapidly and is difficult to resect. Gemcitabine (GEM) as a single agent or in conjunction with radiation is the most commonly used in the management of PaCa. But GEM has shown efficacy only in a small but select group of patients. While the role of key transporters and enzymes has been implicated in sensitizing or conferring resistance to gemcitabine, no clear correlation has been establishe. Currently, there is no a priori way to determine invasively or non-invasively which PaCa patients stand to benefit from GEM therapy. Any biomarker that can act as a prognostic indicator of GEM response will greatly aid in optimizing treatment regimen, reducing unnecessary side effects and subjecting resistant patients to aggressive therapies. Our goal is to develop a PET imaging based biomarker to predict response to GEM therapy in pancreatic cancer patients non-invasively. [18F]-FAC was evaluated as biomarker for GEM response in leukemia models but the short half life (t1/2 = 110 min) combined with background gut activity can complicate image analysis. Therefore our goal was to develop a longer lived analog of GEM that can act as a surrogate marker. Based on modeling studies and ability to label with longer lived isotope (Iodine-124; t1/2 = 4.18 d) we concentrated our efforts on evaluating I-124 labeled 1-(2-Deoxy-2-fluoro-β-D-arabinofuranosyl)-5-iodocytosine ([124I]-FIAC) as a positron emission tomography (PET) biomarker of GEM response. [124I]-FIAC was synthesized by iodination of 1-(2-Deoxy-2-fluoro-β-D-arabinofuranosyl)-cytosine (FAC) with [124I]-NaI using chloramine-T as an oxidant. In vitro phosphorylation efficacy studies were carried out on GEM, FAC and FIAC using recombinant deoxycytidine kinase (dCK) enzyme. In vitro kinetic uptake assay was performed on representattive pancreatic cancer cells lines AsPc-1 and MiaPaCa-2. Subcutaneous tumor xenografts were established in athymic nude mice. [124I]-FIAC was administered intravenously via tail vein and its uptake was studied by PET imaging and sacrificial biodistribution studies at 4, 24, 48 and 72 h. Imaging and biodistribution studies using [18F]-FAC were also performed in tumor bearing mice at 1 and 4 h. [124I]-FIAC was synthesized in >17% yields with >99% radiochemical purity. The efficiency of phosphorylation was in the following order GEM ∼ FAC > FIAC. Cellular uptake assays showed that [124I]-FIAC was taken up preferentially (4X) by AsPc-1 in comparison to MiaPaCa-2. [124I]-FIAC and [18F]-FAC were synthesized and compared for their efficacy to serve as potential biomarker for gemcitabine response in pancreatic cancer models in vitro and in vivo. Preliminary studies indicated that [124I]-FIAC and [18F]-FAC behave differently in these models with former showing preferential uptake in AsPC-1 cells and xenografts. Citation Format: Kishore K. Gangangari, Blesida Punzalan, Brendan Huang, NagaVaraKishore Pillarsetty. Comparison of [124I]-FIAC and [18F]-FAC as potential biomarkers to predict response to gemcitabine therapy in pancreatic cancers. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 5202.

Published

2016

36. Synthesis and biological evaluation of a fluorine-18 derivative of dasatinib

Author

Christophe Antczak, Peter Smith-Jones, Hakim Djaballah, C Lambek, Bayard D. Clarkson, Blesida Punzalan, Darren R. Veach, Elmer Santos, Nagavarakishore Pillarsetty, Steven M. Larson, Mohammad Namavari, and Tatiana Beresten-Kochetkov

Subjects

Fluorine Radioisotopes, Transplantation, Heterologous, Dasatinib, Fusion Proteins, bcr-abl, Mice, Nude, Mice, Growth factor receptor, hemic and lymphatic diseases, Catalytic Domain, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Cell Proliferation, ABL, Chemistry, Kinase, Radiosynthesis, Protein-Tyrosine Kinases, Transplantation, Proto-Oncogene Proteins c-kit, Thiazoles, Pyrimidines, src-Family Kinases, Biochemistry, Positron-Emission Tomography, Cancer research, Molecular Medicine, Radiopharmaceuticals, Tyrosine kinase, medicine.drug, Proto-oncogene tyrosine-protein kinase Src

Abstract

Tyrosine kinases often play pivotal roles in the pathogenesis of cancer and are good candidates for therapeutic intervention and targeted molecular imaging. The precursor synthesis, radiosynthesis, and biological characterization of a fluorine-18 analog of dasatinib, a multitargeted kinase inhibitor, are reported. Compound 5 potently inhibits Abl, Src, and Kit kinases and inhibits K562 and M07e/p210bcr-abl human leukemic cell growth. Using positron emission tomography, we visualized K562 tumor xenografts in mice with [18F]-5.

Published

2007

37. Abstract 5444: Development of a noninvasive assay to determine drug concentration in tumor during hsp90 inhibitor therapy

Author

Efsevia Vakiani, Radu I Peter, Gabriela Chiosis, Nagavarakishore Pillarsetty, Mei H. Chen, Mohammad Nasir Uddin, Adriana D. Corben, Jacek Koziorowski, Smit K. Shah, Tony Taldone, Clifford A. Hudis, Alexander Bolaender, Jason S. Lewis, Thomas Ku, John F. Gerecitano, Elmer Santos, Komal Jhaveri, Pengrong Yan, Christina Pressl, Steven M. Larson, Brad Beattie, Eloisi Caldas-Lopes, Oscar Lin, Yanlong Kang, Anna Rodina, Shanu Modi, Anson Ku, Pat Zanzonico, Yelena Y. Janjigian, Blesida Punzalan, Erica DaGama Gomes, and Mark Dunphy

Subjects

Drug, Cancer Research, business.industry, media_common.quotation_subject, Phases of clinical research, Cancer, Context (language use), medicine.disease, Hsp90 inhibitor, Clinical trial, Oncology, Pharmacokinetics, Biochemistry, medicine, Cancer research, business, media_common, Companion diagnostic

Abstract

As molecularly targeted agents assume a more prominent role in anticancer therapy there is a growing need to determine in a noninvasive manner whether the target is being engaged and to what extent such drug-target binding results in desirable effects. We address this need in the context of Hsp90, a target of significant value and one in critical need for such assessment tools, by combining a novel chemical tool selective for tumor Hsp90 with PET imaging and mathematical modeling. The chemical tool is [124I]-PU-H71, the iodine-124 radiolabeled analog of the potent Hsp90 inhibitor PU-H71, which can be administered in tracer quantities for PET imaging. The resulting diagnostic, PU-PET, has been optimized and validated preclinically in mouse models of cancer and then translated to the clinic. The exquisite design of this assay is based on three essential concepts as it relates to the target (Hsp90) as well as to the PET tracer (124I-PU-H71). First, the target is “oncogenic” Hsp90 and has been shown by numerous biochemical and pharmacokinetic studies to have a strong affinity for inhibitors and a very low koff resulting in selective and prolonged retention in tumor. Secondly, the tracer incorporates a 124I in place of the naturally occurring 127I in the structure of PU-H71 and therefore there is no change in the chemical structure. This feature in a PET tracer intended as a companion diagnostic is unprecedented and ensures that the PK properties are identical to the therapeutic agent (PU-H71). Finally, the radionuclide 124I has a four-day half-life and thus is well-suited to monitor the extended tumor retention profile observed for Hsp90 inhibitors. We here demonstrate that this PET assay informs on Hsp90 targeting in individual tumors in real time and provides accurate tumor drug concentrations for at least four chemically distinct Hsp90 drugs. In contrast, we find that plasma pharmacokinetics is not predictive of intratumor parameters and therefore provides limited value in estimating target engagement. Using PU-PET we demonstrate that at least one Hsp90 inhibitor exhibits tumor targeting and retention in humans, delivering and retaining therapeutic, micromolar, concentrations at safe doses. PU-PET is currently being evaluated in Phase 0/1 (NCT01269593) clinical trials as a noninvasive companion diagnostic to determine intratumoral concentration as well as to identify those patients who would best benefit from Hsp90 inhibitor therapy. This diagnostic assay is intended to be incorporated into future Phase 2 clinical trials in order to preselect those patients who would most likely benefit from Hsp90 inhibitor treatment. Citation Format: Tony Taldone, Nagavarakishore Pillarsetty, Mark PS Dunphy, John F. Gerecitano, Eloisi Caldas-Lopes, Brad Beattie, Radu I. Peter, Yanlong Kang, Anna Rodina, Pengrong Yan, Erica M. DaGama Gomes, Alexander Bolaender, Christina Pressl, Blesida Punzalan, Anson Ku, Thomas Ku, Smit Shah, Mohammad Uddin, Mei H. Chen, Elmer Santos, Jacek Koziorowski, Adriana Corben, Shanu Modi, Komal Jhaveri, Oscar Lin, Efsevia Vakiani, Yelena Janjigian, Pat Zanzonico, Clifford Hudis, Steven M. Larson, Jason S. Lewis, Gabriela Chiosis. Development of a noninvasive assay to determine drug concentration in tumor during hsp90 inhibitor therapy. [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 5444. doi:10.1158/1538-7445.AM2015-5444

Published

2015

38. TU-F-12A-01: Quantitative Non-Linear Compartment Modeling of 89Zr- and 124I- Labeled J591 Monoclonal Antibody Kinetics Using Serial Non-Invasive Positron Emission Tomography Imaging in a Pre-Clinical Human Prostate Cancer Mouse Model

Author

Pat Zanzonico, Steven M. Larson, Blesida Punzalan, Sandhya Chalasani, Edward K. Fung, Sarah M. Cheal, Shoaib B. Fareedy, John L. Humm, Neil H. Bander, B Otto, and Joseph R. Osborne

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, biology, Chemistry, media_common.quotation_subject, medicine.medical_treatment, Cancer, General Medicine, medicine.disease, Prostate cancer, Antigen, Cancer immunotherapy, Positron emission tomography, Radioimmunotherapy, medicine, Cancer research, biology.protein, Antibody, Internalization, media_common

Abstract

Purpose: To examine the binding kinetics of human IgG monoclonal antibody J591 which targets prostate-specific membrane antigen (PSMA) in a pre-clinical mouse cancer model using quantitative PET compartmental analysis of two radiolabeled variants. Methods: PSMA is expressed in normal human prostate, and becomes highly upregulated in prostate cancer, making it a promising therapeutic target. Two forms of J591, radiolabeled with either 8 9Zr or 12 4I, were prepared. 8 9Zr is a radiometal that becomes trapped in the cell upon internalization by the antigen-antibody complex, while radioiodine leaves the cell. Mice with prostate cancer xenografts underwent non-invasive serial imaging on a Focus 120 microPET up to 144 hours post-injection of J591. A non-linear compartmental model describing the binding and internalization of antibody in tumor xenograft was developed and applied to the PET-derived time-activity curves. The antibody-antigen association rate constant (ka), total amount of antigen per gram tumor (Ag_total), internalization rate of antibody-antigen complex, and efflux rate of radioisotope from tumor were fitted using the model. The surface-bound and the internalized activity were also estimated. Results: Values for ka, Ag_total, and internalization rate were found to be similar regardless of radiolabel payload used. The efflux rate, however, was ∼ 9-fold higher for 12 4I-J591 than for 8 9Zr-J591. Time-dependent surface-bound and internalized radiotracer activity were similar for both radiolabels at early times post-injection, but clearly differed beyond 24 hours. Conclusion: Binding and internalization of J591 to PSMA-expressing tumor xenografts were similar when radiolabeled with either 8 9Zr or 12 4I payload. The difference in efflux of radioactivity from tumor may be attributable to differential biological fate intracellularly of the radioisotopes. This has great significance for radioimmunotherapy and antibody-drug conjugates. Further exploration using the model will examine binding and radioisotope residence as antibody dose is increased to antigen saturation. The Center for Targeted Radioimmunotherapy and Theranostics, Ludwig Center for Cancer Immunotherapy, Memorial Sloan Kettering Cancer Center (MSK), NIH (R25-CA096945). Technical services provided by the MSK Small-Animal Imaging Core Facility were supported by the NIH (R24-CA83084, P30-CA08748, and P50-CA92629; Zanzonico). NCI, Center to Reduce Cancer Health Disparity (R21 CA153177-03; Osborne).

Published

2014

39. Sensitive In Vivo Detection of Primary T Cells Expressing Membrane-Anchored Gaussia Luciferase for the Study of Adoptive T Cell Immunotherapy in Murine Models of Malignancy

Author

Yan Nikhamin, Michel Sadelain, Steven M. Larson, Krista M.D. La Perle, Ricardo Toledo-Crow, Renier J. Brentjens, David Entenberg, Elmer Santos, Iana Aranda, Blesida Punzalan, Bleserene Punzalan, and Raymond Yeh

Subjects

Severe combined immunodeficiency, biology, T cell, Immunology, Cell Biology, Hematology, medicine.disease, Biochemistry, Molecular biology, CD19, Chimeric antigen receptor, medicine.anatomical_structure, In vivo, medicine, biology.protein, Luciferase, CD8, Homing (hematopoietic)

Abstract

Current approaches to in vivo bioluminescent imaging (BLI) of T cells utilizing luciferase enzymes may be compromised by poor transduction efficiencies in primary T cells, and low photon emissions. Here we describe a novel and widely applicable approach to in vivo BLI of primary T cells utilizing a membrane-anchored form of the naturally secreted Guassia luciferase (GLuc) enzyme, termed exGLuc. We constructed exGLuc by fusion of the GLuc gene to the coding region of the CD8 transmembrane domain. The resulting exGLuc enzyme is anchored to the cell surface of retrovirally transduced cells. In vitro, cells which expressed the exGLuc enzyme demonstrated a markedly (>9 fold) increased bioluminescent signal when compared to cells which expressed the native GLuc (GLuc), the related Rhenilla luciferase (RLuc), a membrane-anchored form of RLuc (exRLuc), or a green fluorescent protein (GFP)-fire fly luciferase fusion protein. Following injection into SCID-Beige mice, MHC-mismatched C57BL6 T cells transduced to express exGLuc were detected by BLI generating graft versus host disease at an earlier time point and demonstrated a >10 fold increased bioluminescent signal when compared to infused C57BL6 T cells expressing GLuc, RLuc, or exRLuc. We further demonstrate homing of OVA-specific DO11.10 exGLuc+ T cells to A20(OVA) but not A20(GFP) subcutaneous tumors in both SCID-Beige and Balb/c mice. We further successfully applied this strategy to the study of in vivo human T cell homing using a xenogeneic SCID-Beige tumor model. Specifically, we demonstrate that human T cells, retrovirally co-transduced to express both a CD19-specific chimeric antigen receptor (CAR), 19z1, and exGLuc, could be monitored over time, and that these T cells quite rapidly home to subcutaneous CD19+ acute lymphoblastic leukemia (NALM-6) tumors when compared to T cells co-expressing an irrelevant CAR with exGLuc. Furthermore, we were able to demonstrate for the first time specific homing of 19z1/exGLuc+ human T cells to systemic NALM-6 tumor, detecting exGLuc+ T cells in deep tissues including the bone marrow, spleen, and liver. We conclude that the exGLuc enzyme emits a superior bioluminescent signal when compared to other commonly utilized luciferase enzymes; that primary T cells are readily transduced to express the exGLuc enzyme; and that exGLuc+ T cells may be accurately monitored in vivo over time by BLI. Based on these data, we believe that this novel approach to primary T cell in vivo imaging will significantly enhance the study of adoptive T cell immunotherapy in murine models of leukemia and other malignancies.

Published

2006

40. Targeting of radiolabeled J591 antibody to PSMA-expressing tumors: optimization of imaging and therapy based on non-linear compartmental modeling

Author

Jawaria Amir, Daniel E. Spratt, Blesida Punzalan, Sandhya Chalasani, Darren R. Veach, Joseph R. Osborne, Neil H. Bander, Volkan Beylergil, Sarah M. Cheal, Shoaib B. Fareedy, Steven M. Larson, Edward K. Fung, Wolfgang A. Weber, and Pat Zanzonico

Subjects

Pathology, medicine.medical_specialty, media_common.quotation_subject, medicine.medical_treatment, ImmunoPET, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Antigen, LNCaP, PSMA, Medicine, Radiology, Nuclear Medicine and imaging, Internalization, Receptor, Original Research, media_common, medicine.diagnostic_test, biology, business.industry, Iodine-124, Zirconium-89, Non-linear kinetic model, 3. Good health, Monoclonal Antibody J591, Positron emission tomography, 030220 oncology & carcinogenesis, Radioimmunotherapy, Cancer research, biology.protein, J591, Antibody, business

Abstract

Background We applied a non-linear immunokinetic model to quantitatively compare absolute antibody uptake and turnover in subcutaneous LNCaP human prostate cancer (PCa) xenografts of two radiolabeled forms of the humanized anti-prostate-specific membrane antigen (PSMA) monoclonal antibody J591 (124I-J591 and 89Zr-J591). Using the model, we examined the impact of dose on the tumor and plasma positron emission tomography (PET)-derived time-activity curves. We also sought to predict the optimal targeting index (ratio of integrated-tumor-to-integrated-plasma activity concentrations) for radioimmunotherapy. Methods The equilibrium rates of antibody internalization and turnover in the tumors were derived from PET images up to 96 h post-injection using compartmental modeling with a non-linear transfer rate. In addition, we serially imaged groups of LNCaP tumor-bearing mice injected with 89Zr-J591 antibody doses ranging from antigen subsaturating to saturating to examine the suitability of using a non-linear approach and derived the time-integrated concentration (in μM∙hours) of administered tracer in tumor as a function of the administered dose of antibody. Results The comparison of 124I-J591 and 89Zr-J591 yielded similar model-derived values of the total antigen concentration and internalization rate. The association equilibrium constant (ka) was twofold higher for 124I, but there was a ~tenfold greater tumoral efflux rate of 124I from tumor compared to that of 89Zr. Plots of surface-bound and internalized radiotracers indicate similar behavior up to 24 h p.i. for both 124I-J591 and 89Zr-J591, with the effect of differential clearance rates becoming apparent after about 35 h p.i. Estimates of J591/PSMA complex turnover were 3.9–90.5 × 1012 (for doses from 60 to 240 μg) molecules per hour per gram of tumor (20 % of receptors internalized per hour). Conclusions Using quantitative compartmental model methods, surface binding and internalization rates were shown to be similar for both 124I-J591 and 89Zr-J591 forms, as expected. The large difference in clearance rates of the radioactivity from the tumor is likely due to differential trapping of residualizing zirconium versus non-residualizing iodine. Our non-linear model was found to be superior to a conventional linear model. This finding and the calculated activity persistence time in tumor have important implications for radioimmunotherapy and other antibody-based therapies in patients.