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1. Randomized Phase II Trial Comparing Bevacizumab Plus Carboplatin and Paclitaxel With Carboplatin and Paclitaxel Alone in Previously Untreated Locally Advanced or Metastatic Non-Small-Cell Lung Cancer

Author

David H. Johnson, Roy S. Herbst, Corey J. Langer, Louis Fehrenbacher, William Novotny, Eric Holmgren, Jacques Gaudreault, John Nemunaitis, David M. Jablons, Fairooz F. Kabbinavar, Russell F. DeVore, and Lisa A. Damico

Subjects
Male, medicine.medical_specialty, Cancer Research, Lung Neoplasms, Bevacizumab, Paclitaxel, Urology, Antibodies, Monoclonal, Humanized, Carboplatin, chemistry.chemical_compound, Carcinoma, Non-Small-Cell Lung, Antineoplastic Combined Chemotherapy Protocols, medicine, Carcinoma, Motesanib, Humans, Lung cancer, Proportional Hazards Models, Dose-Response Relationship, Drug, business.industry, Area under the curve, Antibodies, Monoclonal, medicine.disease, Survival Analysis, Surgery, chemistry, Oncology, Female, business, medicine.drug, Necitumumab
Abstract

Purpose To investigate the efficacy and safety of bevacizumab plus carboplatin and paclitaxel in patients with advanced or recurrent non-small-cell lung cancer. Patients and Methods In a phase II trial, 99 patients were randomly assigned to bevacizumab 7.5 (n = 32) or 15 mg/kg (n = 35) plus carboplatin (area under the curve = 6) and paclitaxel (200 mg/m2) every 3 weeks or carboplatin and paclitaxel alone (n = 32). Primary efficacy end points were time to disease progression and best confirmed response rate. On disease progression, patients in the control arm had the option to receive single-agent bevacizumab 15 mg/kg every 3 weeks. Results Compared with the control arm, treatment with carboplatin and paclitaxel plus bevacizumab (15 mg/kg) resulted in a higher response rate (31.5% v 18.8%), longer median time to progression (7.4 v 4.2 months) and a modest increase in survival (17.7 v 14.9 months). Of the 19 control patients that crossed over to single-agent bevacizumab, five experienced stable disease, and 1-year survival was 47%. Bleeding was the most prominent adverse event and was manifested in two distinct clinical patterns; minor mucocutaneous hemorrhage and major hemoptysis. Major hemoptysis was associated with squamous cell histology, tumor necrosis and cavitation, and disease location close to major blood vessels. Conclusion Bevacizumab in combination with carboplatin and paclitaxel improved overall response and time to progression in patients with advanced or recurrent non-small-cell lung cancer. Patients with nonsquamous cell histology appear to be a subpopulation with improved outcome and acceptable safety risks.

Published
2023

2. Data from Effects of Anti-VEGF Treatment Duration on Tumor Growth, Tumor Regrowth, and Treatment Efficacy

Author

Greg D. Plowman, Oliver Rosen, Beth Hollister, Germaine Fuh, Maike Schmidt, Hong Xiang, Lisa A. Damico, Ian Kasman, Mallika Singh, Bert Gunter, Leanne Berry, and Anil Bagri

Abstract

Purpose: Inhibition of the vascular endothelial growth factor (VEGF) axis is the basis of all currently approved antiangiogenic therapies. In preclinical models, anti-VEGF blocking antibodies have shown broad efficacy that is dependent on both tumor context and treatment duration. We aimed to characterize this activity and to evaluate the effects of discontinuation of treatment on the dynamics of tumor regrowth.Experimental Design: We evaluated the effects of anti-VEGF treatment on tumor growth and survival in 30 xenograft models and in genetic mouse models of cancer. Histologic analysis was used to evaluate the effects of treatment on tumor vasculature. We used a variety of treatment regimens to allow analysis of the effects of treatment duration and cessation on growth rate, survival, and vascular density.Results: Preclinical tumor models were characterized for their varied dependence on VEGF, thereby defining models for testing other agents that may complement or augment anti-VEGF therapy. We also found that longer exposure to anti-VEGF monoclonal antibodies delayed tumor growth and extended survival in established tumors from both cell transplants and genetic tumor models and prevented regrowth of a subset of residual tumors following cytoablative therapy. Discontinuation of anti-VEGF in established tumors resulted in regrowth at a rate slower than that in control-treated animals, with no evidence of accelerated tumor growth or rebound. However, more rapid regrowth was observed following discontinuation of certain chemotherapies. Concurrent administration of anti-VEGF seemed to normalize these accelerated growth rates.Conclusions: In diverse preclinical models, continuous VEGF suppression provides maximal benefit as a single agent, combined with chemotherapy, or as maintenance therapy once chemotherapy has been stopped. Clin Cancer Res; 16(15); 3887–900. ©2010 AACR.

Published
2023

5. Supplementary Figure 2 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 20K, Effects of 30D8 on 4T1 cell migration in vitro.

Published
2023

6. Supplementary Figure 3 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 239K, Intervention studies in the laser-induced choroidal neovascularization (CNV) model.

Published
2023

10. Supplementary Figure 5 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 28K, Effects of 30D8 on CXCL12 and VEGF serum levels in HM7 tumor bearing mice.

Published
2023

11. Supplementary Figure Legends from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 78K

Published
2023

12. Supplementary Figure 1 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 869K, Proliferation and apoptosis analysis by IF staining in EL4 tumor sections.

Published
2023

13. Supplementary Figure 6 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 26K, Comparison of PK in Balb c/nude mice of three hamster antibodies with similar binding affinity toward human CXCL12.

Published
2023

14. Supplementary Figure 4 from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

PDF file, 38K, Sequence alignment of 30D8 and humanized 30D8 (hu30D8).

Published
2023

15. Supplementary Figure 6 from Onartuzumab (MetMAb): Using Nonclinical Pharmacokinetic and Concentration–Effect Data to Support Clinical Development

Author

Lisa A. Damico-Beyer, Amy Peterson, Judy Young, Elaine Mai, Ihsan Nijem, Teresa Davancaze, Mally Romero, Nelson L. ‘Shasha’ Jumbe, Mark Merchant, Arthur E. Reyes, Brendan C. Bender, and Hong Xiang

Abstract

PDF file, 2424K, Observed individual concentration-time profile of onartuzumab in human in comparison with cyno-based prediction.

Published
2023

18. Data from Onartuzumab (MetMAb): Using Nonclinical Pharmacokinetic and Concentration–Effect Data to Support Clinical Development

Author

Lisa A. Damico-Beyer, Amy Peterson, Judy Young, Elaine Mai, Ihsan Nijem, Teresa Davancaze, Mally Romero, Nelson L. ‘Shasha’ Jumbe, Mark Merchant, Arthur E. Reyes, Brendan C. Bender, and Hong Xiang

Abstract

Purpose: We characterized the pharmacokinetics of onartuzumab (MetMAb) in animals and determined a concentration–effect relationship in tumor-bearing mice to enable estimation of clinical pharmacokinetics and target doses.Experimental Design: A tumor growth inhibition model was used to estimate tumoristatic concentrations (TSC) in mice. Human pharmacokinetic parameters were projected from pharmacokinetics in cynomolgus monkeys by the species-invariant time method. Monte Carlo simulations predicted the percentage of patients achieving steady-state trough serum concentrations (Ctrough ss) ≥TSC for every 3-week (Q3W) dosing.Results: Onartuzumab clearance (CL) in the linear dose range was 21.1 and 12.2 mL/d/kg in mice and cynomolgus monkeys with elimination half-life at 6.10 and 3.37 days, respectively. The estimated TSC in KP4 pancreatic xenograft tumor-bearing mice was 15 μg/mL. Projected CL for humans in the linear dose range was 5.74 to 9.36 mL/d/kg with scaling exponents of CL at 0.75 to 0.9. Monte Carlo simulations projected a Q3W dose of 10 to 30 mg/kg to achieve Ctrough ss of 15 μg/mL in 95% or more of patients.Conclusions: Onartuzumab pharmacokinetics differed from typical bivalent glycosylated monoclonal antibodies with approximately 2-times faster CL in the linear dose range. Despite this higher CL, xenograft efficacy data supported dose flexibility with Q1W to Q3W dose regimens in the clinical setting with a TSC of 15 μg/mL as the Ctrough ss target. The projected human efficacious dose of 10 to 30 mg/kg Q3W should achieve the target TSC of 15 μg/mL. These data show effective pharmacokinetic/pharmacodynamic modeling to project doses to be tested in the clinic. Clin Cancer Res; 19(18); 5068–78. ©2013 AACR.

Published
2023

20. Data from Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Napoleone Ferrara, Weiru Wang, Robert F. Kelley, Camellia Adams, Richard D. Carano, Lisa A. Damico-Beyer, Wyne P. Lee, Rashi Takkar, Jenny Yao, Racquel Corpuz, Kai Barck, Eric Suto, Peter Gribling, Leah Quintana, Robyn Clark, Suzy Clark, Nancy Y. Chiang, Terence Wong, Mary Coons, Mark Ultsch, Hong Xiang, Bing Li, Jianyong Wang, and Cuiling Zhong

Abstract

Purpose: Our goal was to develop a potent humanized antibody against mouse/human CXCL12. This report summarized its in vitro and in vivo activities.Experimental Design: Cell surface binding and cell migration assays were used to select neutralizing hamster antibodies, followed by testing in several animal models. Monoclonal antibody (mAb) 30D8 was selected for humanization based on its in vitro and in vivo activities.Results: 30D8, a hamster antibody against mouse and human CXCL12α, CXCL12β, and CXCL12γ, was shown to dose-dependently block CXCL12α binding to CXCR4 and CXCR7, and CXCL12α-induced Jurkat cell migration in vitro. Inhibition of primary tumor growth and/or metastasis was observed in several models. 30D8 alone significantly ameliorated arthritis in a mouse collagen-induced arthritis model (CIA). Combination with a TNF-α antagonist was additive. In addition, 30D8 inhibited 50% of laser-induced choroidal neovascularization (CNV) in mice. Humanized 30D8 (hu30D8) showed similar in vitro and in vivo activities as the parental hamster antibody. A crystal structure of the hu30D8 Fab/CXCL12α complex in combination with mutational analysis revealed a “hot spot” around residues Asn44/Asn45 of CXCL12α and part of the RFFESH region required for CXCL12α binding to CXCR4 and CXCR7. Finally, hu30D8 exhibited fast clearance in cynomolgus monkeys but not in rats.Conclusion: CXCL12 is an attractive target for treatment of cancer and inflammation-related diseases; hu30D8 is suitable for testing this hypothesis in humans. Clin Cancer Res; 19(16); 4433–45. ©2013 AACR.

Published
2023

25. Supplementary Figure Legends 1-6 from A Therapeutic Anti–VEGF Antibody with Increased Potency Independent of Pharmacokinetic Half-life

Author

Henry B. Lowman, Napoleone Ferrara, Lisa A. Damico, Y. Gloria Meng, William F. Forrest, Mauricio Maia, John Lowe, Samantha Lien, Jean-Michel Vernes, Arthur E. Reyes, Xiumin Wu, and Yik Andy Yeung

Abstract

Supplementary Figure Legends 1-6 from A Therapeutic Anti–VEGF Antibody with Increased Potency Independent of Pharmacokinetic Half-life

Published
2023

29. Pharmacokinetics and biodistribution of a human monoclonal antibody to oxidized LDL in cynomolgus monkey using PET imaging.

Author

Amrita V Kamath, Simon P Williams, Sherry Bullens, Kyra J Cowan, Yvonne Stenberg, Simon R Cherry, Stephen Rendig, David L Kukis, Chris Griesemer, Lisa A Damico-Beyer, and Stuart Bunting

Subjects
Medicine, Science
Abstract

Oxidized low-density lipoprotein (LDL) plays an essential role in the pathogenesis of atherosclerosis. The purpose of this study was to characterize the pharmacokinetics (PK) of a human recombinant IgG1 antibody to oxidized LDL (anti-oxLDL) in cynomolgus monkey. The tissue biodistribution of anti-oxLDL was also investigated using positron emission tomography (PET) imaging.Anti-oxLDL was conjugated with the N-hydroxysuccinimide ester of DOTA (1,4,7,10-tetraazacyclododecane 1,4,7,10-tetraacetic acid) and radiolabeled by chelation of radioactive copper-64 ((64)Cu) for detection by PET. Anti-oxLDL was administered as a single intravenous (IV) dose of 10 mg/kg (as a mixture of radiolabeled and non-labeled material) to two male and two female cynomolgus monkeys. Serum samples were collected over 29 days. Two ELISA methods were used to measure serum concentrations of anti-oxLDL; Assay A was a ligand binding assay that measured free anti-oxLDL (unbound and partially bound forms) and Assay B measured total anti-oxLDL. The biodistribution was observed over a 48-hour period following dose administration using PET imaging.Anti-oxLDL serum concentration-time profiles showed a biphasic elimination pattern that could be best described by a two-compartment elimination model. The serum concentrations obtained using the two ELISA methods were comparable. Clearance values ranged from 8 to 17 ml/day/kg, while beta half-life ranged from 8 to 12 days. The initial volume of distribution and volume of distribution at steady state were approximately 55 mL/kg and 150 mL/kg, respectively. PET imaging showed distribution predominantly to the blood pool, visible as the heart and great vessels in the trunk and limbs, plus diffuse signals in the liver, kidney, spleen, and bone marrow.The clearance of anti-oxLDL is slightly higher than typical IgG1 antibodies in cynomolgus monkeys. The biodistribution pattern appears to be consistent with an antibody that has no large, rapid antigen sink outside the blood space.

Published
2012
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30. Dose dependent pharmacokinetics, tissue distribution, and anti-tumor efficacy of a humanized monoclonal antibody against DLL4 in mice

Author

Victor Yip, Leslie A. Khawli, C. Andrew Boswell, Joni Castro, Sarajane Ross, Ben-Quan Shen, Lisa A. Damico-Beyer, Amrita V. Kamath, Priyanka Gupta, Glenn Pacheco, Peter Haughney, Siao Ping Tsai, Daniela Bumbaca, and Minhong Yan

Subjects
Lung Neoplasms, Metabolic Clearance Rate, medicine.drug_class, tissue distribution, Immunology, Mice, Nude, DLL4, Pharmacology, Antibodies, Monoclonal, Humanized, Monoclonal antibody, Iodine Radioisotopes, Pharmacokinetics, antibody, Cell Line, Tumor, medicine, cancer, Animals, Humans, Immunology and Allergy, Tissue distribution, Lung, Dose-Response Relationship, Drug, biology, Dose dependent pharmacokinetics, Indium Radioisotopes, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Cancer, Ligand (biochemistry), medicine.disease, Xenograft Model Antitumor Assays, Treatment Outcome, medicine.anatomical_structure, Area Under Curve, Immunoglobulin G, cardiovascular system, biology.protein, Female, Antibody, pharmacokinetics, Reports
Abstract

Delta-like-4 ligand (DLL4) plays an important role in vascular development and is widely expressed on the vasculature of normal and tumor tissues. Anti-DLL4 is a humanized IgG1 monoclonal antibody against DLL4. The purpose of these studies was to characterize the pharmacokinetics (PK), tissue distribution, and anti-tumor efficacy of anti-DLL4 in mice over a range of doses. PK and tissue distribution of anti-DLL4 were determined in athymic nude mice after administration of single intravenous (IV) doses. In the tissue distribution study, radiolabeled anti-DLL4 (mixture of (125)Iodide and (111)Indium) was administered in the presence of increasing amounts of unlabeled anti-DLL4. Dose ranging anti-DLL4 anti-tumor efficacy was evaluated in athymic nude mice bearing MV522 human lung tumor xenografts. Anti-DLL4 had nonlinear PK in mice with rapid serum clearance at low doses and slower clearance at higher doses suggesting the involvement of target mediated clearance. Consistent with the PK data, anti-DLL4 was shown to specifically distribute to several normal tissues known to express DLL4 including the lung and liver. Maximal efficacy in the xenograft model was seen at doses ≥ 10 mg/kg when tissue sinks were presumably saturated, consistent with the PK and tissue distribution profiles. These findings highlight the importance of mechanistic understanding of antibody disposition to enable dosing strategies for maximizing efficacy.

Published
2014

31. Complement Inhibition in Cynomolgus Monkeys by Anti–Factor D Antigen-Binding Fragment for the Treatment of an Advanced Form of Dry Age-Related Macular Degeneration

Author

Kelly M. Loyet, Lisa A. Damico-Beyer, Jeremy Good, Kha Le, Xiangdan Wang, Philip E. Hass, Laura DeForge, Teresa Davancaze, Jihong Yang, Alyssa Morimoto, Lizette Sturgeon, Menno van Lookeren Campagne, Maureen Wong, and Peter Haughney

Subjects
Male, Pharmacology, Lampalizumab, Immunoglobulin Fab Fragments, Macular Degeneration, Mice, medicine, Animals, Humans, Antigen Binding Fragment, Serine protease, Dose-Response Relationship, Drug, biology, business.industry, Macular degeneration, medicine.disease, Complement inhibition, Macaca fascicularis, Dose–response relationship, Treatment Outcome, Intravitreal Injections, Immunology, Complement C3a, biology.protein, Alternative complement pathway, Molecular Medicine, Cattle, Complement Factor D, Female, Factor D, business
Abstract

Anti-factor D (AFD; FCFD4514S, lampalizumab) is a humanized IgG Fab fragment directed against factor D (fD), a rate-limiting serine protease in the alternative complement pathway (AP). Evaluation of AFD as a potential intravitreal (IVT) therapeutic for dry age-related macular degeneration patients with geographic atrophy (GA) is ongoing. However, it is unclear whether IVT administration of AFD can affect systemic AP activation and potentially compromise host-immune responses. We characterized the pharmacologic properties of AFD and assessed the effects of AFD administered IVT (2 or 20 mg) or intravenous (0.2, 2, or 20 mg) on systemic complement activity in cynomolgus monkeys. For the IVT groups, serum AP activity was reduced for the 20 mg dose group between 2 and 6 hours postinjection. For the intravenous groups, AFD inhibited systemic AP activity for periods of time ranging from 5 minutes (0.2 mg group) to 3 hours (20 mg group). Interestingly, the concentrations of total serum fD increased up to 10-fold relative to predose levels following administration of AFD. Furthermore, AFD was found to inhibit systemic AP activity only when the molar concentration of AFD exceeded that of fD. This occurred in cynomolgus monkeys at serum AFD levels ≥2 µg/ml, a concentration 8-fold greater than the maximum serum concentration observed following a single 10 mg IVT dose in a clinical investigation in patients with GA. Based on these findings, the low levels of serum AFD resulting from IVT administration of a clinically relevant dose are not expected to appreciably affect systemic AP activity.

Published
2014

32. Onartuzumab (MetMAb): Using Nonclinical Pharmacokinetic and Concentration–Effect Data to Support Clinical Development

Author

Hong Xiang, Mally Romero, Lisa A. Damico-Beyer, Judy Young, Mark Merchant, Elaine Mai, Amy C. Peterson, Ihsan Nijem, Nelson L. Jumbe, Brendan C. Bender, Arthur E. Reyes, and Teresa Davancaze

Subjects
Cancer Research, Blotting, Western, Mice, Nude, Pharmacology, Immunoenzyme Techniques, Mice, Pharmacokinetics, Predictive Value of Tests, Tumor Cells, Cultured, Animals, Humans, Immunoprecipitation, Computer Simulation, Tissue Distribution, Dosing, Dose-Response Relationship, Drug, Chemistry, Antibodies, Monoclonal, Half-life, Serum concentration, Xenograft Model Antitumor Assays, Pancreatic Neoplasms, Macaca fascicularis, Dose–response relationship, Oncology, Onartuzumab, Pharmacodynamics, Tumor growth inhibition, Female, Monte Carlo Method, Carcinoma, Pancreatic Ductal, Half-Life
Abstract

Purpose: We characterized the pharmacokinetics of onartuzumab (MetMAb) in animals and determined a concentration–effect relationship in tumor-bearing mice to enable estimation of clinical pharmacokinetics and target doses. Experimental Design: A tumor growth inhibition model was used to estimate tumoristatic concentrations (TSC) in mice. Human pharmacokinetic parameters were projected from pharmacokinetics in cynomolgus monkeys by the species-invariant time method. Monte Carlo simulations predicted the percentage of patients achieving steady-state trough serum concentrations (Ctrough ss) ≥TSC for every 3-week (Q3W) dosing. Results: Onartuzumab clearance (CL) in the linear dose range was 21.1 and 12.2 mL/d/kg in mice and cynomolgus monkeys with elimination half-life at 6.10 and 3.37 days, respectively. The estimated TSC in KP4 pancreatic xenograft tumor-bearing mice was 15 μg/mL. Projected CL for humans in the linear dose range was 5.74 to 9.36 mL/d/kg with scaling exponents of CL at 0.75 to 0.9. Monte Carlo simulations projected a Q3W dose of 10 to 30 mg/kg to achieve Ctrough ss of 15 μg/mL in 95% or more of patients. Conclusions: Onartuzumab pharmacokinetics differed from typical bivalent glycosylated monoclonal antibodies with approximately 2-times faster CL in the linear dose range. Despite this higher CL, xenograft efficacy data supported dose flexibility with Q1W to Q3W dose regimens in the clinical setting with a TSC of 15 μg/mL as the Ctrough ss target. The projected human efficacious dose of 10 to 30 mg/kg Q3W should achieve the target TSC of 15 μg/mL. These data show effective pharmacokinetic/pharmacodynamic modeling to project doses to be tested in the clinic. Clin Cancer Res; 19(18); 5068–78. ©2013 AACR.

Published
2013

33. Development and Preclinical Characterization of a Humanized Antibody Targeting CXCL12

Author

Camellia W. Adams, Cuiling Zhong, Kai H. Barck, Terence Wong, Wyne P. Lee, Suzy Clark, Weiru Wang, Racquel Corpuz, Mary Coons, Bing Li, Richard A.D. Carano, Rashi Takkar, Nan Chiang, Leah Quintana, Peter Gribling, Hong Xiang, Robyn Clark, Jenny Yao, Jianyong Wang, Mark Ultsch, Robert F. Kelley, Napoleone Ferrara, Eric Suto, and Lisa A. Damico-Beyer

Subjects
Models, Molecular, Vascular Endothelial Growth Factor A, Cancer Research, Protein Conformation, medicine.drug_class, Anti-Inflammatory Agents, Drug Evaluation, Preclinical, Hamster, Angiogenesis Inhibitors, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, Monoclonal antibody, Humanized antibody, Mice, In vivo, Cell Line, Tumor, Cricetinae, Neoplasms, medicine, Animals, Humans, Neoplasm Metastasis, biology, Antibodies, Monoclonal, Drug Synergism, Arthritis, Experimental, Xenograft Model Antitumor Assays, Molecular biology, Chemokine CXCL12, In vitro, Tumor Burden, Disease Models, Animal, Epitope mapping, Oncology, Monoclonal, biology.protein, Cancer research, Female, Antibody, Epitope Mapping
Abstract

Purpose: Our goal was to develop a potent humanized antibody against mouse/human CXCL12. This report summarized its in vitro and in vivo activities. Experimental Design: Cell surface binding and cell migration assays were used to select neutralizing hamster antibodies, followed by testing in several animal models. Monoclonal antibody (mAb) 30D8 was selected for humanization based on its in vitro and in vivo activities. Results: 30D8, a hamster antibody against mouse and human CXCL12α, CXCL12β, and CXCL12γ, was shown to dose-dependently block CXCL12α binding to CXCR4 and CXCR7, and CXCL12α-induced Jurkat cell migration in vitro. Inhibition of primary tumor growth and/or metastasis was observed in several models. 30D8 alone significantly ameliorated arthritis in a mouse collagen-induced arthritis model (CIA). Combination with a TNF-α antagonist was additive. In addition, 30D8 inhibited 50% of laser-induced choroidal neovascularization (CNV) in mice. Humanized 30D8 (hu30D8) showed similar in vitro and in vivo activities as the parental hamster antibody. A crystal structure of the hu30D8 Fab/CXCL12α complex in combination with mutational analysis revealed a “hot spot” around residues Asn44/Asn45 of CXCL12α and part of the RFFESH region required for CXCL12α binding to CXCR4 and CXCR7. Finally, hu30D8 exhibited fast clearance in cynomolgus monkeys but not in rats. Conclusion: CXCL12 is an attractive target for treatment of cancer and inflammation-related diseases; hu30D8 is suitable for testing this hypothesis in humans. Clin Cancer Res; 19(16); 4433–45. ©2013 AACR.

Published
2013

34. Population pharmacokinetic and pharmacodynamic modeling of MNRP1685A in cynomolgus monkeys using two-target quasi-steady-state (QSS) model

Author

Hong Xiang, Denise Jin, Frank-Peter Theil, Amita Joshi, Yan Xin, Lisa A. Damico-Beyer, and Shuang Bai

Subjects
Male, Population, Central compartment, Pharmacology, Models, Biological, Drug Delivery Systems, Elimination rate constant, Pharmacokinetics, Animals, Humans, Medicine, education, education.field_of_study, Sheep, Dose-Response Relationship, Drug, business.industry, Antibodies, Monoclonal, Neuropilin-1, Macaca fascicularis, Dose–response relationship, Immunoglobulin G, Pharmacodynamics, Blood vessel maturation, Female, business, Dose selection
Abstract

MNRP1685A (anti-NRP1) is a fully human IgG1 monoclonal antibody against neuropilin-1 (NRP1), a protein necessary for blood vessel maturation. MNRP1685A binds to free membrane-bound NRP1 (mNRP1) and circulating NRP1 (cNRP1). Total cNRP1 increased in a dose-dependent manner following anti-NRP1 administration in mice, rats, and monkeys. The purpose of this study is to develop a mechanism-based model to simultaneously describe the kinetics of both unbound drug (MNRP1685A) and total cNRP1 in cynomolgus monkeys. Pharmacokinetic (PK) and pharmacodynamic (PD) profiles after single- or multiple-dose administrations were well described by the two-target quasi-steady-state (QSS) model. The estimated nonspecific clearance was 3.26 mL/day/kg and central compartment volume was 38.2 mL/kg. The maximum elimination rate for mNRP1-mediated disposition was 98.8 nM/day. The synthesis rate (3.8 nM/day), degradation rate constant (1.53 day(-1)), and complex elimination rate constant (0.260 day(-1)) for cNRP1 were also derived from the model. QSS constants were 6.94 nM for mNRP1 and 2.8 nM for cNRP1. The results suggest that cNRP1 has minimal effect on MNRP1685A PK while mNRP1 plays a major role in the target-mediated drug disposition. This finding is favorable as the desired pharmacological target is mNRP1, rather than cNRP1. The two-target QSS model provides mechanistic understanding of the nonlinear PK of MNRP1685A. Based on the model prediction, the free drug concentrations to maintain free mNRP1 and cNRP1 below 10% of baseline level are 10 and 20 μg/mL, respectively. This serves as a target concentration for clinical dose selection, assuming cynomolgus monkeys are predictive for humans.

Published
2012

35. Identification of circulating neuropilin-1 and dose-dependent elevation following anti-neuropilin-1 antibody administration

Author

Ryan J. Watts, Wendy Sandoval, Yanmei Lu, Alexander W. Koch, Raymond K. Tong, Peter Liu, Lisa A Damico, Y. Gloria Meng, Wai Lee Wong, and Hong Xiang

Subjects
medicine.medical_specialty, Angiogenesis, medicine.drug_class, Blotting, Western, Immunology, Enzyme-Linked Immunosorbent Assay, Monoclonal antibody, Mice, chemistry.chemical_compound, Western blot, Report, Cricetinae, Internal medicine, Neuropilin 1, medicine, Extracellular, Animals, Humans, Immunology and Allergy, Dose-Response Relationship, Drug, biology, medicine.diagnostic_test, Antibodies, Monoclonal, Neuropilin-1, Rats, Blot, Vascular endothelial growth factor, Endocrinology, Gene Expression Regulation, chemistry, biology.protein, Antibody
Abstract

Neuropilin-1 (NRP1) acts as a co-receptor for class 3 semaphorins and vascular endothelial growth factor and is an attractive angiogenesis target for cancer therapy. In addition to the transmembrane form, naturally occurring soluble NRP1 proteins containing part of the extracellular domain have been identified in tissues and a cell line. We developed ELISAs to study the existence of circulating NRP1 and to quantify it in serum. As measured by ELISAs, circulating NRP1 levels in mice, rats, monkeys and humans were 427 +/- 77, 20 +/- 3, 288 +/- 86 and 322 +/- 82 ng/ml (mean +/- standard deviation; n > or = 10), respectively. Anti-NRP1(B), a human monoclonal antibody, has been selected from a synthetic phage library. A 4-fold increase in circulating NRP1 was observed in mice receiving a single dose of 10 mg/kg anti-NRP1(B) antibody. In rats and monkeys receiving single injections of anti-NRP1(B) at different dose levels, higher doses of antibody resulted in greater and more prolonged increases in circulating NRP1. Maximum increases were 56- and 7-fold for rats and monkeys receiving 50 mg/kg anti-NRP1(B), respectively. In addition to the soluble NRP1 isoforms, for the first time, a approximately 120 kDa circulating NRP1 protein containing the complete extracellular domain was detected in serum by western blot and mass spectrometry analysis. This protein increased more than the putative soluble NRP1 bands in anti-NRP1(B) treated mouse, rat and monkey sera compared with untreated controls, suggesting that anti-NRP1(B) induced membrane NRP1 shedding.

Published
2009

36. A mechanistic pharmacokinetic/pharmacodynamic model of factor D inhibition in cynomolgus monkeys by lampalizumab for the treatment of geographic atrophy

Author

Teresa Davancaze, Leonid Gibiansky, Jin Jin, William D. Hanley, Kelly M. Loyet, Jeremy Good, Alyssa Morimoto, Kha Le, Menno van Lookeren Campagne, and Lisa A. Damico-Beyer

Subjects
Male, Biodistribution, Phases of clinical research, Pharmacology, Antibodies, Monoclonal, Humanized, Models, Biological, Lampalizumab, Retina, Aqueous Humor, Immunoglobulin Fab Fragments, Pharmacokinetics, Geographic Atrophy, Medicine, Animals, biology, business.industry, Intravitreal administration, Vitreous Body, Macaca fascicularis, Pharmacodynamics, Immunology, Intravitreal Injections, biology.protein, Alternative complement pathway, Molecular Medicine, Factor D, Administration, Intravenous, Complement Factor D, Female, business
Abstract

Lampalizumab is an antigen-binding fragment of a humanized monoclonal antibody against complement factor D (CFD), a rate-limiting enzyme in the activation and amplification of the alternative complement pathway (ACP), which is in phase III clinical trials for the treatment of geographic atrophy. Understanding of the pharmacokinetics, pharmacodynamics, and biodistribution of lampalizumab following intravitreal administration in the ocular compartments and systemic circulation is limited but crucial for selecting doses that provide optimal efficacy and safety. Here, we sought to construct a semimechanistic and integrated ocular-systemic pharmacokinetic-pharmacodynamic model of lampalizumab in the cynomolgus monkey to provide a quantitative understanding of the ocular and systemic disposition of lampalizumab and CFD inhibition. The model takes into account target-mediated drug disposition, target turnover, and drug distribution across ocular tissues and systemic circulation. Following intravitreal administration, lampalizumab achieves rapid equilibration across ocular tissues. Lampalizumab ocular elimination is relatively slow, with a τ1/2 of approximately 3 days, whereas systemic elimination is rapid, with a τ1/2 of 0.8 hours. Target-independent linear clearance is predominant in the eye, whereas target-mediated clearance is predominant in the systemic circulation. Systemic CFD synthesis was estimated to be high (7.8 mg/day); however, the amount of CFD entering the eye due to influx from the systemic circulation was small (

Published
2015

37. DEVELOPMENT OF RANIBIZUMAB, AN ANTI–VASCULAR ENDOTHELIAL GROWTH FACTOR ANTIGEN BINDING FRAGMENT, AS THERAPY FOR NEOVASCULAR AGE-RELATED MACULAR DEGENERATION

Author

Lisa A. Damico, Naveed Shams, Robert Kim, Henry B. Lowman, and Napoleone Ferrara

Subjects
Vascular Endothelial Growth Factor A, Oncology, medicine.medical_specialty, Visual acuity, genetic structures, Angiogenesis, Pegaptanib, Visual Acuity, Angiogenesis Inhibitors, Antibodies, Monoclonal, Humanized, Immunoglobulin Fab Fragments, Macular Degeneration, chemistry.chemical_compound, Ranibizumab, Ophthalmology, Internal medicine, medicine, Humans, Randomized Controlled Trials as Topic, business.industry, Antibodies, Monoclonal, General Medicine, Macular degeneration, medicine.disease, Choroidal Neovascularization, eye diseases, Vascular endothelial growth factor, Vascular endothelial growth factor A, Choroidal neovascularization, chemistry, medicine.symptom, business, medicine.drug
Abstract

Background Angiogenesis is a key aspect of the wet form of age-related neovascular (AMD), the leading cause of blindness in the elderly population. Substantial evidence indicated that vascular endothelial growth factor (VEGF)-A is a major mediator of angiogenesis and vascular leakage in wet AMD. VEGF-A is the prototype member of a gene family that includes also PlGF, VEGF-B, VEGF-C, VEGF-D and the orf virus-encoded VEGF-E. Several isoforms of VEGF-A can be generated due to alternative mRNA splicing. Various VEGF inhibitors have been clinically developed. Among these, ranibizumab is a high affinity recombinant Fab that neutralizes all isoforms of VEGF-A. The article briefly reviews the biology of VEGF and then focuses on the path that led to clinical development of ranibizumab. Results The safety and efficacy of ranibizumab in the treatment of neovascular AMD have been evaluated in two large phase III, multicenter, randomized, double-masked, controlled pivotal trials in different neovascular AMD patient populations. Combined, the trial results indicate that ranibizumab results not only in a slowing down of vision loss but also in a significant proportion of patients experiencing a clinically meaningful vision gain. The visual acuity benefit over control was observed regardless of CNV lesion type. Furthermore, the benefit was associated with a low rate of serious adverse events. Conclusions Ranibizumab represents a novel therapy that, for the first time, appears to have the potential to enable many AMD patients to obtain a meaningful and sustained gain of vision. On June 30 2006, ranibizumab was approved by the US Food and Drug Administration for the treatment of wet AMD.

Published
2006

38. A Phase II Study of Thalidomide in Advanced Metastatic Renal Cell Carcinoma

Author

Gloria Meng, Dana Monroe, Laurence Elias, David R. Minor, Lisa A. Damico, and Uma Suryadevara

Subjects
Adult, Male, Vascular Endothelial Growth Factor A, Pathology, medicine.medical_specialty, Angiogenesis, medicine.medical_treatment, Disorders of Excessive Somnolence, Endothelial Growth Factors, chemistry.chemical_compound, Renal cell carcinoma, Carcinoma, Humans, Medicine, Pharmacology (medical), Carcinoma, Renal Cell, Aged, Pharmacology, Lymphokines, Chemotherapy, Kidney, Vascular Endothelial Growth Factors, business.industry, Middle Aged, medicine.disease, Kidney Neoplasms, Thalidomide, Vascular endothelial growth factor, Vascular endothelial growth factor A, medicine.anatomical_structure, Oncology, chemistry, Cancer research, Intercellular Signaling Peptides and Proteins, Female, sense organs, business, Constipation, medicine.drug
Abstract

To evaluate the toxicity and activity of thalidomide in patients with advanced metastatic renal cell cancer and to measure changes of one angiogenic factor, vascular endothelial growth factor (VEGF)165, with therapy.29 patients were enrolled on a study of thalidomide using an intra-patient dose escalation schedule. Patients began thalidomide at 400 mg/d and escalated as tolerated to 1200 mg/d by day 54. Fifty-nine per cent of patients had had previous therapy with IL-2 and 52% were performance status 2 or 3. Systemic plasma VEGF165 levels were measured by dual monoclonal ELISA in 8 patients.24 patients were evaluable for response with one partial response of 11 months duration of a patient with hepatic and pulmonary metastases (4%), one minor response, and 2 patients stable for over 6 months. Somnolence and constipation were prominent toxicities and most patients could not tolerate the 1200 mg/day dose level. Systemic plasma VEGF165 levels did not change with therapy.These results are consistent with a low level of activity of thalidomide in renal cell carcinoma. Administration of doses over 800 mg/day was difficult to achieve in this patient population, however lower doses were practical. The dose-response relationship, if any, of thalidomide for renal cell carcinoma is unclear.

Published
2002

39. Albumin Binding as a General Strategy for Improving the Pharmacokinetics of Proteins

Author

Min Zhang, Daniel Kirchhofer, Mark S. Dennis, Miryam Kadkhodayan, Y. Gloria Meng, Dan Combs, and Lisa A. Damico

Subjects
Phage display, Molecular Sequence Data, Serum albumin, Peptide, Plasma protein binding, Biochemistry, Mice, Animals, Humans, Bacteriophages, Amino Acid Sequence, Binding site, Molecular Biology, Peptide sequence, Serum Albumin, chemistry.chemical_classification, Binding Sites, Sequence Homology, Amino Acid, biology, Chemistry, Albumin, Proteins, Cell Biology, Surface Plasmon Resonance, Rats, biology.protein, Rabbits, Small molecule binding, Half-Life, Protein Binding
Abstract

Plasma protein binding can be an effective means of improving the pharmacokinetic properties of otherwise short lived molecules. Using peptide phage display, we identified a series of peptides having the core sequence DICLPRWGCLW that specifically bind serum albumin from multiple species with high affinity. These peptides bind to albumin with 1:1 stoichiometry at a site distinct from known small molecule binding sites. Using surface plasmon resonance, the dissociation equilibrium constant of peptide SA21 (Ac-RLIEDICLPRWGCLWEDD-NH(2)) was determined to be 266 +/- 8, 320 +/- 22, and 467 +/- 47 nm for rat, rabbit, and human albumin, respectively. SA21 has an unusually long half-life of 2.3 h when injected by intravenous bolus into rabbits. A related sequence, fused to the anti-tissue factor Fab of D3H44 (Presta, L., Sims, P., Meng, Y. G., Moran, P., Bullens, S., Bunting, S., Schoenfeld, J., Lowe, D., Lai, J., Rancatore, P., Iverson, M., Lim, A., Chisholm, V., Kelley, R. F., Riederer, M., and Kirchhofer, D. (2001) Thromb. Haemost. 85, 379-389), enabled the Fab to bind albumin with similar affinity to that of SA21 while retaining the ability of the Fab to bind tissue factor. This interaction with albumin resulted in reduced in vivo clearance of 25- and 58-fold in mice and rabbits, respectively, when compared with the wild-type D3H44 Fab. The half-life was extended 37-fold to 32.4 h in rabbits and 26-fold to 10.4 h in mice, achieving 25-43% of the albumin half-life in these animals. These half-lives exceed those of a Fab'(2) and are comparable with those seen for polyethylene glycol-conjugated Fab molecules, immunoadhesins, and albumin fusions, suggesting a novel and generic method for improving the pharmacokinetic properties of rapidly cleared proteins.

Published
2002

40. Vascular Endothelial Growth Factor KDR Receptor Signaling Potentiates Tumor Necrosis Factor-induced Tissue Factor Expression in Endothelial Cells

Author

Thomas F. Zioncheck, Ben-Quan Shen, Karen M. Cortopassi, Lisa A. Damico, and David Y. Lee

Subjects
Vascular Endothelial Growth Factor A, medicine.medical_specialty, Endothelial Growth Factors, Biochemistry, Thromboplastin, chemistry.chemical_compound, Tissue factor, Proto-Oncogene Proteins, Internal medicine, Neuropilin, medicine, Humans, Receptors, Growth Factor, Enzyme Inhibitors, Growth Substances, Molecular Biology, Cells, Cultured, Protein Kinase C, Protein kinase C, Lymphokines, Vascular Endothelial Growth Factor Receptor-1, Tumor Necrosis Factor-alpha, Vascular Endothelial Growth Factors, Chemistry, Receptor Protein-Tyrosine Kinases, Drug Synergism, Kinase insert domain receptor, Cell Biology, Protein-Tyrosine Kinases, Staurosporine, Genistein, Molecular biology, Up-Regulation, Vascular endothelial growth factor, Vascular endothelial growth factor A, Receptors, Vascular Endothelial Growth Factor, Endocrinology, Mutation, cardiovascular system, Tumor necrosis factor alpha, Endothelium, Vascular, Signal transduction, Signal Transduction
Abstract

Vascular endothelial growth factor (VEGF) and tumor necrosis factor-alpha (TNF-alpha) have been shown to synergistically increase tissue factor (TF) expression in endothelial cells; however, the role of the VEGF receptors (KDR, Flt-1, and neuropilin) in this process is unclear. Here we report that VEGF binding to the KDR receptor is necessary and sufficient for the potentiation of TNF-induced TF expression in human umbilical vein endothelial cells. TF expression was evaluated by Western blot analysis and fluorescence-activated cell sorting. In the absence of TNF-alpha, wild-type VEGF- or KDR receptor-selective variants induced an approximate 7-fold increase in total TF expression. Treatment with TNF alone produced an approximate 110-fold increase in total TF expression, whereas coincubation of TNF-alpha with wild-type VEGF- or KDR-selective variants resulted in an approximate 250-fold increase in TF expression. VEGF lacking the heparin binding domain was also able to potentiate TF expression, indicating that heparin-sulfate proteoglycan or neuropilin binding is not required for TF up-regulation. Neither placental growth factor nor an Flt-1-selective variant was capable of inducing TF expression in the presence or absence of TNF. Inhibition of protein-tyrosine kinase or protein kinase C activity significantly blocked the TNF/VEGF potentiation of TF up-regulation, whereas phorbol 12-myristate 13-acetate, a protein kinase C activator, increased TF expression. These data demonstrate that KDR receptor signaling governs both VEGF-induced TF expression and the potentiation of TNF-induced up-regulation of TF.

Published
2001

41. Population pharmacokinetic analysis from phase I and phase II studies of the humanized monovalent antibody, onartuzumab (MetMAb), in patients with advanced solid tumors

Author

John Bothos, Lisa A. Damico-Beyer, Surinder Kaur, Amita Joshi, Ihsan Nijem, Shuang Bai, Yan Xin, Stephen Eppler, Denise Jin, Amy C. Peterson, John D. Davis, and Premal Patel

Subjects
Pharmacology, education.field_of_study, Chemistry, medicine.drug_class, Population, Phases of clinical research, Renal function, Monoclonal antibody, Onartuzumab, Pharmacokinetics, medicine, Pharmacology (medical), Dosing, Erlotinib, education, medicine.drug
Abstract

Onartuzumab is a unique, humanized, monovalent (one-armed) monoclonal antibody (mAb) against the MET receptor. The intravenous (IV) pharmacokinetics (PK) of onartuzumab were investigated in a phase I study and a phase II study in recurrent non-small cell lung cancer (NSCLC) patients. The potential for drug-drug interaction (DDI) was assessed during co-administration of IV onartuzumab with oral erlotinib, by measuring the PK of both drugs. The concentration-time profiles of onartuzumab were adequately described using a two-compartment model with linear clearance (CL) at doses between 4 and 30 mg/kg. The estimates for CL, central compartment volume (V1 ), and median terminal half-life were 0.439 L/day, 2.77 L, and 13.4 days, respectively. Statistically significant covariates included creatinine clearance (CrCL) on clearance, weight and gender on V1 , and weight on peripheral compartment volume (V2 ), but the clinical relevance of these covariates needs to be further evaluated. The current analysis did not indicate obvious DDI between onartuzumab and erlotinib. MET diagnostic status did not impact the exposure of either agent. Despite the slightly faster clearance compared with typical bivalent mAbs, the PK of onartuzumab support dosing regimens of 15 mg/kg every 3 weeks or doses equivalent to achieve the target minimum tumoristatic concentration in patients.

Published
2013

42. Death receptor 5 agonistic antibody PRO95780: preclinical pharmacokinetics and concentration-effect relationship support clinical dose and regimen selection

Author

Lisa A. Damico-Beyer, Sean K. Kelley, Steve Eppler, Hong Xiang, and Arthur E. Reyes

Subjects
Cancer Research, Mice, Nude, Enzyme-Linked Immunosorbent Assay, Pharmacology, Toxicology, Antibodies, Monoclonal, Humanized, Mice, Pharmacokinetics, Cell Line, Tumor, Medicine, Animals, Humans, Pharmacology (medical), PK/PD models, Models, Statistical, biology, Dose-Response Relationship, Drug, business.industry, Half-life, Antibodies, Monoclonal, Xenograft Model Antitumor Assays, Rats, Regimen, Dose–response relationship, Macaca fascicularis, Receptors, TNF-Related Apoptosis-Inducing Ligand, Oncology, Pharmacodynamics, Area Under Curve, Monoclonal, Injections, Intravenous, biology.protein, Female, Antibody, business, Neoplasm Transplantation, Half-Life
Abstract

PRO95780, a human monoclonal antibody (mAb) against death receptor 5 (DR5/TRAIL-R2/TNFRSF10B), was developed for the treatment for cancer. Our objective was to characterize pharmacokinetics (PK) in mice, rats, and cynomolgus monkeys and concentration–effect relationships of PRO95780 in xenograft mouse models of human cancers; this would guide the selection of dose and regimen for clinical trials. The PK profiles were determined in mice, rats, and cynomolgus monkeys. Three xenograft models with a wide range of in vitro sensitivities to PRO95780 were selected for efficacy studies. Tumoristatic serum concentrations (TSCs) were determined using PK/pharmacodynamic (PD) modeling with tumor growth as a PD endpoint. A species-invariant time PK scaling method was employed to estimate disposition in humans using PK data in cynomolgus monkeys. Furthermore, the predicted human PK parameters were used to estimate dose and regimen to achieve TSC observed in mice at the steady-state trough concentrations (C trough ss) in the clinic. Linear PK was observed across species. A serum concentration of 22 μg/mL was identified to be the target TSC in mice. A dose of 10 mg/kg administered once every 2 weeks (Q2W) was predicted to achieve a TSC at C trough ss in 95 % of patients. PRO95780 has linear PK in mice, rats, and monkeys. Estimated TSCs varied among different xenograft models. A projected target dose in humans is achievable for Q2W administration within the dose range used for other commercial mAbs.

Published
2013

43. Chemical Versus Isotopic Equilibrium and the Metabolic Fate of Glycolytic End Products in the Heart

Author

Lisa A. Damico, Lawrence T. White, Xin Yu, and Douglas E. Lewandowski

Subjects
Alanine, Pyruvate decarboxylation, Magnetic Resonance Spectroscopy, Cahill cycle, Chemistry, Myocardium, Oxidative phosphorylation, Metabolism, In Vitro Techniques, Citric acid cycle, chemistry.chemical_compound, Biochemistry, Lactate dehydrogenase, Animals, Glycolysis, Rabbits, Hypoxia, Cardiology and Cardiovascular Medicine, Molecular Biology
Abstract

Recent studies of isotope exchange across lactate dehydrogenase (LDH) and alanine aminotransferase (AAT) in hearts call into question whether both reactions are in equilibrium. To compare the oxidative and non-oxidative fates of glycolytic end products, isolated rabbit hearts were perfused with 5 mM [2-13C] glucose and 2.5 mM [3-13C] pyruvate: with (n = 6) and without (n = 7) stimulation of pyruvate oxidation using dichloroacetate (DCA), and during normal perfusion or hypoxia (n = 7/n = 6, +/- DCA). 13C NMR spectroscopy of intact hearts confirmed a steady-state enrichment level in both alanine and lactate. 1H- and 13C-NMR spectroscopy of tissue extracts identified the fractions of lactate, alanine and glutamate pools formed from each exogenous substrate. Glycolysis from glucose accounted for 22 +/- 7% of lactate formed and 10 +/- 2% of alanine formed in control hearts, and 16 +/- 2% lactate and 15 +/- 2% alanine in hypoxic hearts (mean +/- S.E.M.). In contrast, exogenous pyruvate formed 36 +/- 5% of the lactate pool, and 86 +/- 3% of the alanine pool in controls and 47 +/- 3% of lactate and of 67 +/- 3% alanine during hypoxia. [2(-13)C] glucose did not contribute to oxidative energy production via the TCA cycle as determined from low 13C enrichment of glutamate C5 from glucose (< 2%), while [3-13C] pyruvate accounted for 84 +/- 7% of labeled glutamate C4. Thus, exogenous pyruvate out-competed the metabolism of glucose, indicating low glycolytic activity. At 40 min, 96 +/- 2% of the total alanine was labeled from either glucose or pyruvate, confirming equilibrium at AAT. However, only 55 +/- 10% of total lactate was labeled, suggesting that the LDH reaction is not in rapid equilibrium within the myocardium.

Published
1996

44. Multiplet structure of13C NMR signal from glutamate and direct detection of tricarboxylic acid (TCA) cycle intermediates

Author

Chris Doumen, Kathryn F. LaNoue, Lawrence T. White, Xin Yu, Lisa A. Damico, and E. Douglas Lewandowski

Subjects
chemistry.chemical_classification, Magnetic Resonance Spectroscopy, Myocardium, Citric Acid Cycle, Succinic Acid, Glutamate receptor, Glutamic Acid, Succinates, Nuclear magnetic resonance spectroscopy, Tricarboxylic acid, In Vitro Techniques, Carbon-13 NMR, Isotopomers, Citric acid cycle, chemistry.chemical_compound, chemistry, Biochemistry, Succinic acid, Animals, Ketoglutaric Acids, Radiology, Nuclear Medicine and imaging, Rabbits, Steady state (chemistry)
Abstract

For the first time, 13C NMR signals are shown from 13C-enriched, low-level tricarboxylic acid (TCA) cycle intermediates from extracts of normal cardiac tissue. As the low tissue content of the key intermediates alpha-ketoglutarate (alpha-KG) and succinate (SUC) in normal, well perfused tissues has until now precluded direct NMR detection from intact tissues and tissue extracts, 13C NMR signal from glutamate has generally been used to infer the isotopomer patterns of intermediates that are in chemical exchange with glutamate. However, the required assumptions regarding intracellular compartmentation for such indirect analysis have not been previously tested, as glutamate is largely cytosolic while the TCA cycle enzymes are located in the mitochondria. Chromatographic isolation of alpha-KG and SUC from heart tissue extracts allowed isotopomer analysis to be performed for comparison with that of glutamate. At steady state, a direct relationship between glutamate and alpha-ketoglutarate isotopomers was found, but succinate isotopomers matched those of glutamate only in hearts that displayed negligible contributions from the oxidation of unlabeled endogenous carbon sources.

Published
1996

45. Kinetic analysis of dynamic 13C NMR spectra: metabolic flux, regulation, and compartmentation in hearts

Author

Lisa A. Damico, Kathryn F. LaNoue, Nathaniel M. Alpert, E. D. Lewandowski, Xin Yu, Lawrence T. White, and Chris Doumen

Subjects
Magnetic Resonance Spectroscopy, Stereochemistry, Citric Acid Cycle, Biophysics, Glutamic Acid, chemistry.chemical_element, Butyrate, Acetates, In Vitro Techniques, 030204 cardiovascular system & hematology, Models, Biological, Oxygen, Biophysical Phenomena, Butyric acid, 03 medical and health sciences, chemistry.chemical_compound, Acetic acid, Oxygen Consumption, 0302 clinical medicine, Animals, Aspartate Aminotransferases, Acetic Acid, 030304 developmental biology, Carbon Isotopes, 0303 health sciences, Chemistry, Myocardium, Nuclear magnetic resonance spectroscopy, Glutamic acid, Carbon-13 NMR, Myocardial Contraction, Perfusion, Butyrates, Kinetics, Butyric Acid, Rabbits, Oxidation-Reduction, Flux (metabolism), Research Article, Nuclear chemistry
Abstract

Control of oxidative metabolism was studied using 13C NMR spectroscopy to detect rate-limiting steps in 13C labeling of glutamate. 13C NMR spectra were acquired every 1 or 2 min from isolated rabbit hearts perfused with either 2.5 mM [2-13C]acetate or 2.5 mM [2-13C]butyrate with or without KCl arrest. Tricarboxylic acid cycle flux (VTCA) and the exchange rate between alpha-ketoglutarate and glutamate (F1) were determined by least-square fitting of a kinetic model to NMR data. Rates were compared to measured kinetics of the cardiac glutamate-oxaloacetate transaminase (GOT). Despite similar oxygen use, hearts oxidizing butyrate instead of acetate showed delayed incorporation of 13C label into glutamate and lower VTCA, because of the influence of beta-oxidation: butyrate = 7.1 +/- 0.2 mumol/min/g dry wt; acetate = 10.1 +/- 0.2; butyrate + KCl = 1.8 +/- 0.1; acetate + KCl = 3.1 +/- 0.1 (mean +/- SD). F1 ranged from a low of 4.4 +/- 1.0 mumol/min/g (butyrate + KCl) to 9.3 +/- 0.6 (acetate), at least 20-fold slower than GOT flux, and proved to be rate limiting for isotope turnover in the glutamate pool. Therefore, dynamic 13C NMR observations were sensitive not only to TCA cycle flux but also to the interconversion between TCA cycle intermediates and glutamate.

Published
1995
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46. Cardiac responses to induced lactate oxidation: NMR analysis of metabolic equilibria

Author

Lisa A. Damico, Lawrence T. White, E. D. Lewandowski, and Xin Yu

Subjects
Pyruvate decarboxylation, Magnetic Resonance Spectroscopy, Physiology, Intracellular pH, Oxidative phosphorylation, In Vitro Techniques, Phosphocreatine, chemistry.chemical_compound, Lactate oxidation, Physiology (medical), Pyruvic Acid, Animals, Lactic Acid, Pyruvates, Carbon Isotopes, Myocardium, Heart, Intracellular Membranes, Metabolism, Nuclear magnetic resonance spectroscopy, Hydrogen-Ion Concentration, Pyruvate dehydrogenase complex, Myocardial Contraction, Carbon, chemistry, Biochemistry, Lactates, Rabbits, Energy Metabolism, Cardiology and Cardiovascular Medicine, Oxidation-Reduction
Abstract

The role of lactate as a source of pyruvate oxidation in supporting cardiac work, energetics, and formation of oxidative metabolites was examined in normal myocardium. 13C- and 31P-nuclear magnetic resonance (NMR) spectra were acquired from isolated rabbit hearts supplied 2.5 mM [3-13C]lactate or [3-13C]pyruvate with or without stimulation of pyruvate dehydrogenase (PDH) by dichloroacetate (DCA). Similar workloads determined by rate-pressure products were noted with pyruvate (21,700 +/- 2,400; mean +/- SE) and lactate (18,970 +/- 1,510). Oxygen consumption was similar in all four groups with means between 19.0 and 22.2 mumol.min-1.g dry weight-1 (SE = 1.6-2.0) as was the ratio of phosphocreatine to ATP with means between 1.8 and 2.1 (SE = 0.1-0.6). Intracellular pH, determined from 31P-NMR spectra, was essentially the same with pyruvate (7.06 +/- 0.02) and lactate (7.05 +/- 0.04). 13C enrichment of glutamate was higher with lactate (92%) than with pyruvate (70%). Pyruvate plus DCA induced no change in glutamate content at 9-10 mumol/g, but 13C enrichment increased to 83%, while lactate plus DCA maintained enrichment at 90%. Levels of alpha-ketoglutarate were lower with lactate (1.81 mumol/g) than with pyruvate (2.36 mumol/g). Lactate plus DCA elevated glutamate by 60% with a proportional increase in alpha-ketoglutarate. Thus the balance between glutamate and alpha-ketoglutarate was affected by substrate supply only and not by PDH activation. The results suggest that the equilibrium between alpha-ketoglutarate and glutamate is sensitive to cytosolic redox state, an important consideration for 13C-NMR analyses that rely on glutamate.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1995

47. A guide to rational dosing of monoclonal antibodies

Author

Mark J. Dresser, Denise Jin, Dan Lu, Yan Xin, Shuang Bai, Lisa A. Damico-Beyer, Karin Jorga, Manish Gupta, Yi Zhang, David E. Allison, Amita Joshi, Meina Tang, and Yanan Zheng

Subjects
Adult, Male, Databases, Factual, Body Surface Area, Metabolic Clearance Rate, Population, Cmax, Pharmacology, Models, Biological, Cmin, Pharmacokinetics, Medicine, Humans, Pharmacology (medical), Computer Simulation, Dosing, education, Volume of distribution, Body surface area, education.field_of_study, Dose-Response Relationship, Drug, business.industry, Body Weight, Decision Trees, Antibodies, Monoclonal, Median body, Female, business
Abstract

Dosing of therapeutic monoclonal antibodies (mAbs) is often based on body size, with the perception that body size-based dosing would reduce inter-subject variability in drug exposure. However, most mAbs are target specific with a relatively large therapeutic window and generally a small contribution of body size to pharmacokinetic variability. Therefore, the dosing paradigm for mAbs should be assessed in the context of these unique characteristics. The objective of this study was to review the current dosing strategy and to provide a scientific rationale for dosing of mAbs using a modelling and simulation approach.In this analysis, the body weight-based or body weight-independent (fixed) dosing regimens for mAbs were systematically evaluated. A generic two-compartment first-order elimination model was developed. Individual or population pharmacokinetic profiles were simulated as a function of the body weight effects on clearance (θ(BW_CL)) and on the central volume of distribution (θ(BW_V1)). The variability in exposure (the area under the serum concentration-time curve [AUC], trough serum concentration [C(min)] and peak serum concentration [C(max)]) was compared between body weight-based dosing and fixed dosing in the entire population. The deviation of exposure for light and heavy subjects from median body weight subjects was also measured. The simulation results were then evaluated with clinical pharmacokinetic characteristics of various mAbs that were given either by body weight-based dosing or by fixed dosing in the case study.Results from this analysis demonstrated that exposure variability was dependent on the magnitude of the body weight effect on pharmacokinetics. In contrast to the conventional assumption, body weight-based dosing does not always offer advantages over fixed dosing in reducing exposure variability. In general, when the exponential functions of θ(BW_CL) and θ(BW_V1) in the population pharmacokinetic model are0.5, fixed dosing results in less variability and less deviation than body weight-based dosing; when both θ(BW_CL) and θ(BW_V1) are0.5, body weight-based dosing results in less variability and less deviation than fixed dosing. In the scenarios when either θ(BW_CL) or θ(BW_V1) is0.5, the impact on exposure variability is different for each exposure measure. The case study demonstrated that most mAbs had little effect or a moderate body weight effect (θ(BW_CL) and θ(BW_V1)0.5 or ∼0.5). The difference of variability in exposure between body weight-based and fixed dosing is generally less than 20% and the percentages of deviation for light and heavy subpopulations are less than 40%.The analysis provided insights into the conditions under which either fixed or body weight-based dosing would be superior in reducing pharmacokinetic variability and exposure differences between light and heavy subjects across the population. The pharmacokinetic variability introduced by either dosing regimen is moderate relative to the variability generally observed in pharmacodynamics, efficacy and safety. Therefore, mAb dosing can be flexible. Given many practical advantages, fixed dosing is recommended to be the first option in first-in-human studies with mAbs. The dosing strategy in later stages of clinical development could then be determined based on combined knowledge of the body weight effect on pharmacokinetics, safety and efficacy from the early clinical trials.

Published
2012

48. Preclinical pharmacokinetics of MFGR1877A, a human monoclonal antibody to FGFR3, and prediction of its efficacious clinical dose for the treatment of t(4;14)-positive multiple myeloma

Author

Jean-Philippe Stephan, Hao Li, Denise Jin, Ann Brady, Lisa A. Damico-Beyer, Jing Qing, Dan Lu, Priyanka Gupta, Janet Tien, Amrita V. Kamath, and Yan Xin

Subjects
musculoskeletal diseases, Cancer Research, medicine.drug_class, Mice, Nude, Pharmacology, Toxicology, Fibroblast growth factor, Monoclonal antibody, Antibodies, Monoclonal, Humanized, Rats, Sprague-Dawley, Mice, Pharmacokinetics, medicine, Animals, Humans, Receptor, Fibroblast Growth Factor, Type 3, Pharmacology (medical), Receptor, Multiple myeloma, biology, business.industry, Antibodies, Monoclonal, Fibroblast growth factor receptor 3, medicine.disease, Xenograft Model Antitumor Assays, Rats, Macaca fascicularis, Oncology, Nonlinear Dynamics, Immunoglobulin G, Monoclonal, biology.protein, Antibody, business, Multiple Myeloma
Abstract

MFGR1877A is a human IgG1 monoclonal antibody that binds to fibroblast growth factor receptor 3 (FGFR3) and is being investigated as a potential therapy for relapsed/refractory FGFR3+ multiple myeloma. The purpose of these studies was to characterize the pharmacokinetics (PK) of MFGR1877A in mouse, rat, and monkey and predict its human PK and efficacious dose.PK of MFGR1877A was determined in athymic nude mice, Sprague-Dawley rats and cynomolgus monkeys after administration of single intravenous doses. Human PK profiles were projected from monkey PK profiles using a species-invariant time method, and human population PK parameters were estimated using a non-linear, two-compartment model comprising specific (target-mediated) and non-specific clearance pathways. The anti-tumor efficacy in mice bearing human tumor xenografts was used in conjunction with inhibitory activity in cell proliferation assays and human PK projections to estimate clinical efficacious dose.The PK of MFGR1877A in mice was non-linear in the dose range of 1-50 mg/kg, while in rats and monkeys, PK was non-linear in the dose range of 1-10 mg/kg and linear at doses ≥ 10 mg/kg. The predicted non-specific clearance range in humans was 2.6-4.4 mL/day/kg. Doses ranging from 2 to 3 mg/kg weekly to 6-10 mg/kg every 4 weeks were predicted to achieve the target exposure in ≥ 90% of multiple myeloma patients.The predicted non-specific clearance of MFGR1877A in humans is similar to typical human IgG1 antibodies and will be verified in a Phase 1 study. The projected human efficacious dose and regimen appear to be achievable in patients.

Published
2011

49. Preclinical pharmacokinetics of MEHD7945A, a novel EGFR/HER3 dual-action antibody, and prediction of its human pharmacokinetics and efficacious clinical dose

Author

Lisa A. Damico-Beyer, Mark X. Sliwkowski, Lisa Crocker, Denise Jin, Cecilia Leddy, Gabriele Schaefer, Amrita V. Kamath, Hong Xiang, Dan Lu, Anne Wong, and Priyanka Gupta

Subjects
Cancer Research, Receptor, ErbB-3, medicine.drug_class, Antineoplastic Agents, Mice, SCID, Pharmacology, Toxicology, Monoclonal antibody, Mice, Pharmacokinetics, Dual action, Preclinical pharmacokinetics, medicine, Animals, Humans, Pharmacology (medical), biology, Dose-Response Relationship, Drug, business.industry, Antibodies, Monoclonal, ErbB Receptors, Macaca fascicularis, Oncology, Immunoglobulin G, biology.protein, Female, Antibody, business, Human cancer
Abstract

MEHD7945A is a novel dual-action monoclonal antibody in which each of the two antigen-binding fragments is capable of binding to EGFR and HER3 with high affinity. It is being evaluated as a potential therapy for human cancer. The purpose of these studies was to characterize the pharmacokinetics (PK) of MEHD7945A in mouse and monkey and predict its human PK and efficacious dose.PK of MEHD7945A was determined in SCID beige mice and cynomolgus monkeys after administration of single intravenous doses. Human PK profiles were projected from monkey PK profiles using a species-invariant time method, and human population PK parameters were estimated using a nonlinear, two-compartment model comprising specific (target-mediated) and nonspecific clearance pathways. The antitumor efficacy in mice bearing human tumor xenografts was used in conjunction with human PK projections to estimate human efficacious doses.The total clearance of MEHD7945A decreased with increase in dose in both mouse and monkey. The nonspecific clearance in monkey was estimated to be 14 mL/day/kg. The predicted nonspecific clearance range in humans was 6-10 mL/day/kg. Doses of 8-12 mg/kg administered every 2 weeks in humans were predicted to achieve exposure of 300 day μg/mL per week to match the efficacious exposure observed in xenograft models.The PK of MEHD7945A was nonlinear in mouse and monkey in the dose range tested. The nonspecific clearance in monkey was approximately twofold higher than typical humanized IgG1 antibodies. The projected human efficacious dose and dose regimen appear to be achievable in patients.

Published
2011

50. Effects of anti-VEGF treatment duration on tumor growth, tumor regrowth, and treatment efficacy

Author

Ian Kasman, Bert Gunter, Maike Schmidt, Germaine Fuh, Beth Hollister, Anil Bagri, Mallika Singh, Oliver Rosen, Leanne Berry, Lisa A. Damico, Hong Xiang, and Greg Plowman

Subjects
Vascular Endothelial Growth Factor A, Cancer Research, Pathology, medicine.medical_specialty, medicine.medical_treatment, Context (language use), Angiogenesis Inhibitors, Cross Reactions, chemistry.chemical_compound, Mice, Maintenance therapy, Cell Line, Tumor, Blocking antibody, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Chemotherapy, Neovascularization, Pathologic, business.industry, Cancer, Antibodies, Monoclonal, Neoplasms, Experimental, medicine.disease, Xenograft Model Antitumor Assays, Discontinuation, Accelerated Growth, Vascular endothelial growth factor, Treatment Outcome, Oncology, chemistry, Cancer research, business
Abstract

Purpose: Inhibition of the vascular endothelial growth factor (VEGF) axis is the basis of all currently approved antiangiogenic therapies. In preclinical models, anti-VEGF blocking antibodies have shown broad efficacy that is dependent on both tumor context and treatment duration. We aimed to characterize this activity and to evaluate the effects of discontinuation of treatment on the dynamics of tumor regrowth. Experimental Design: We evaluated the effects of anti-VEGF treatment on tumor growth and survival in 30 xenograft models and in genetic mouse models of cancer. Histologic analysis was used to evaluate the effects of treatment on tumor vasculature. We used a variety of treatment regimens to allow analysis of the effects of treatment duration and cessation on growth rate, survival, and vascular density. Results: Preclinical tumor models were characterized for their varied dependence on VEGF, thereby defining models for testing other agents that may complement or augment anti-VEGF therapy. We also found that longer exposure to anti-VEGF monoclonal antibodies delayed tumor growth and extended survival in established tumors from both cell transplants and genetic tumor models and prevented regrowth of a subset of residual tumors following cytoablative therapy. Discontinuation of anti-VEGF in established tumors resulted in regrowth at a rate slower than that in control-treated animals, with no evidence of accelerated tumor growth or rebound. However, more rapid regrowth was observed following discontinuation of certain chemotherapies. Concurrent administration of anti-VEGF seemed to normalize these accelerated growth rates. Conclusions: In diverse preclinical models, continuous VEGF suppression provides maximal benefit as a single agent, combined with chemotherapy, or as maintenance therapy once chemotherapy has been stopped. Clin Cancer Res; 16(15); 3887–900. ©2010 AACR.

Published
2010

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