Your search keyword '"Michael W. Bolt"' showing total 12 results

1. Nonclinical Studies that Support Viral Vector-Delivered Gene Therapies: An EFPIA Gene Therapy Working Group Perspective

Author

Peter Ulrich, Michael W. Bolt, Antonio R. Fernández de Henestrosa, Claudette L. Fuller, Prathap Kumar S. Mahalingaiah, David R. Compton, Laurence O. Whiteley, Jessica L. Lynch, Brian Lauritzen, Timothy K. MacLachlan, and Binu K. Philip

Subjects

0301 basic medicine, medicine.medical_specialty, lcsh:QH426-470, Genetic enhancement, Harmonization, Viral vector, Toxicology studies, 03 medical and health sciences, 0302 clinical medicine, Genetics, Medicine, lcsh:QH573-671, Intensive care medicine, Molecular Biology, Gene, Modalities, lcsh:Cytology, business.industry, Safety pharmacology, Perspective (graphical), lcsh:Genetics, 030104 developmental biology, 030220 oncology & carcinogenesis, Molecular Medicine, Original Article, business

Abstract

Nonclinical development strategies for gene therapies are unique from other modalities. The European Federation of Pharmaceutical Industries and Associates (EFPIA) Gene Therapy Working Group surveyed EFPIA member and nonmember pharmaceutical and biotechnology companies about their current practices for designing and implementing nonclinical toxicology studies to support the development of viral vector-delivered in vivo gene therapies. Compiled responses from 17 companies indicated that these studies had some variability in species selection, study-design elements, biodistribution, immunogenicity or genomic insertion assessments, safety pharmacology, and regulatory interactions. Although there was some consistency in general practice, there were examples of extreme case-by-case differences. The responses and variability are discussed herein. Key development challenges were also identified. Results from this survey emphasize the importance for harmonization of regulatory guidelines for the development of gene-therapy products, while still allowing for case-by-case flexibility in nonclinical toxicology studies. However, the appropriate timing for a harmonized guidance, particularly with a platform that continues to rapidly evolve, remains in question., Graphical Abstract, The European Federation of Pharmaceutical Industries and Associates Gene Therapy Working Group conducted a survey on current practices associated with nonclinical toxicity studies conducted to support the development of in vivo viral vector-delivered gene therapies. Responses provide insight on studies conducted, endpoints evaluated, and challenges faced by biopharmaceutical/biotechnology companies.

Published

2020

2. Development challenges associated with rAAV-based gene therapies

Author

Lawrence O Whiteley, K Nasir Khan, Michael W. Bolt, and Joseph T. Brady

Subjects

business.industry, Mechanism (biology), Carcinogenesis, Genetic Vectors, Authorization, Neurotoxicity, Gene Transfer Techniques, Genetic Therapy, 010501 environmental sciences, Dependovirus, Toxicology, Bioinformatics, medicine.disease, 030226 pharmacology & pharmacy, 01 natural sciences, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Mutagenesis, medicine, Humans, Regulatory agency, business, Gene, 0105 earth and related environmental sciences

Abstract

The number of gene therapies in development continues to increase, as they represent a novel method to treat, and potentially cure, many diseases. Gene therapies can be conducted with an in vivo or ex vivo approach, to cause gene augmentation, gene suppression, or genomic editing. Adeno-associated viruses are commonly used to deliver gene therapies, but their use is associated with several manufacturing, nonclinical and clinical challenges. As these challenges emerge, regulatory agency expectations continue to evolve. Following administration of rAAV-based gene therapies, nonclinical toxicities may occur, which includes immunogenicity, hepatotoxicity, neurotoxicity, and the potential risks for insertional mutagenesis and subsequent tumorgenicity. The mechanism for these findings and translation into the clinical setting are unclear at this time but have influenced the nonclinical studies that regulatory agencies are increasingly requesting to support clinical trials and marketing authorizations. These evolving regulatory expectations and toxicities, as well as future nonclinical considerations, are discussed herein.

Published

2021

3. Small Molecule Proprotein Convertase Subtilisin/Kexin Type 9 (PCSK9) Inhibitors: Hit to Lead Optimization of Systemic Agents

Author

Liuqing Wei, Jun Xiao, Joseph S. Warmus, Jeffrey R. Chabot, Robert Dullea, Christopher T. Salatto, David W. Piotrowski, Benjamin A. Thuma, Donna N. Petersen, Chris Limberakis, Julien Genovino, Steven B. Coffey, Michael W. Bolt, Kim F. McClure, Kevin D. Hesp, Spiros Liras, Jamie H. D. Cate, Nathanael G. Lintner, Allyn T. Londregan, Gary Erik Aspnes, and Benjamin Reidich

Subjects

Male, 0301 basic medicine, 01 natural sciences, Rats, Sprague-Dawley, Structure-Activity Relationship, 03 medical and health sciences, In vivo, Drug Discovery, Animals, Structure–activity relationship, Protease Inhibitors, 010405 organic chemistry, Chemistry, PCSK9, PCSK9 Inhibitors, Subtilisin, Hit to lead, Proprotein convertase, Small molecule, Rats, 0104 chemical sciences, 030104 developmental biology, Biochemistry, Drug Design, Molecular Medicine, Kexin, Safety

Abstract

The optimization of a new class of small molecule PCSK9 mRNA translation inhibitors is described. The potency, physicochemical properties, and off-target pharmacology associated with the hit compound (1) were improved by changes to two regions of the molecule. The last step in the synthesis of the congested amide center was enabled by three different routes. Subtle structural changes yielded significant changes in pharmacology and off-target margins. These efforts led to the identification of 7l and 7n with overall profiles suitable for in vivo evaluation. In a 14-day toxicology study, 7l demonstrated an improved safety profile vs lead 7f. We hypothesize that the improved safety profile is related to diminished binding of 7l to nontranslating ribosomes and an apparent improvement in transcript selectivity due to the lower strength of 7l stalling of off-target proteins.

Published

2018

4. Liver-Targeted Small-Molecule Inhibitors of Proprotein Convertase Subtilisin/Kexin Type 9 Synthesis

Author

Dennis O. Scott, Spiros Liras, Roger B. Ruggeri, Heather Eng, Adam S. Kamlet, Ryosuke Arakawa, David W. Piotrowski, Robert Dullea, Christopher T. Salatto, Karen Atkinson, Michael W. Bolt, Anne-Marie R. Dechert-Schmitt, Paul DaSilva-Jardine, Allyn T. Londregan, Brian Raymer, Kenneth Dahl, Daniel P. Canterbury, Donna N. Petersen, Paula M. Loria, Chris Limberakis, Emi Kimoto, Kim F. McClure, Kevin Beaumont, Liuqing Wei, Akihiro Takano, Kevin P. Maresca, Jun Xiao, Amanda King-Ahmad, Christer Halldin, Benjamin Reidich, and Jeffrey R. Chabot

Subjects

0301 basic medicine, Drug, media_common.quotation_subject, Ribosome, Catalysis, Small Molecule Libraries, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Humans, media_common, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, PCSK9, PCSK9 Inhibitors, Subtilisin, General Medicine, General Chemistry, Prodrug, Proprotein convertase, Small molecule, 030104 developmental biology, Liver, Biochemistry, 030220 oncology & carcinogenesis, Hepatocytes, Kexin, Proprotein Convertase 9

Abstract

Targeting of the human ribosome is an unprecedented therapeutic modality with a genome-wide selectivity challenge. A liver-targeted drug candidate is described that inhibits ribosomal synthesis of PCSK9, a lipid regulator considered undruggable by small molecules. Key to the concept was the identification of pharmacologically active zwitterions designed to be retained in the liver. Oral delivery of the poorly permeable zwitterions was achieved by prodrugs susceptible to cleavage by carboxylesterase 1. The synthesis of select tetrazole prodrugs was crucial. A cell-free in vitro translation assay containing human cell lysate and purified target mRNA fused to a reporter was used to identify active zwitterions. In vivo PCSK9 lowering by oral dosing of the candidate prodrug and quantification of the drug fraction delivered to the liver utilizing an oral positron emission tomography 18F-isotopologue validated our liver-targeting approach.

Published

2017

5. Preclinical Pharmacokinetics, Pharmacodynamics, Tissue Distribution, and Interspecies Scaling of Recombinant Human Coagulation Factor Xa I16L

Author

Chuenlei Parng, Boris Gorovits, Rob Webster, Teresa M Caiazzo, Nicole Duriga, Debra D. Pittman, Michael W. Bolt, Alison Joyce, Beth A. Leary, Victoria Markiewicz, Jianqing Chen, and Lisa Dyleski

Subjects

0301 basic medicine, Intracerebral hemorrhage, Biodistribution, Pharmaceutical Science, Plasma protein binding, 030204 cardiovascular system & hematology, Pharmacology, Biology, medicine.disease, law.invention, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Pharmacokinetics, Coagulation, law, Pharmacodynamics, medicine, Recombinant DNA, Distribution (pharmacology)

Abstract

FXaI16L is a recombinant human FXa variant which is currently being evaluated in the clinic for treating intracerebral hemorrhage. The aim of our studies is to investigate overall pharmacokinetics, pharmacodynamics, and distribution of FXaI16L in preclinical species, and to understand its potential implication in human. Pharmacokinetics of FXaI16L was examined using active site probes and the results showed that FXaI16L displayed fast clearance, low volume of distribution, and a very short plasma resident time in mice, rats, and monkeys. When pharmacodynamics was examined in monkeys, concentration effects of FXaI16L on shortening of active partial prothrombin time and formation of thrombin-antithrombin complex were observed. Furthermore, biodistribution study was conducted in mice using radiolabeled FXaI16L, and showed that 125I-FXaI16L has high plasma protein binding and significant liver and kidney distribution. Human pharmacokinetic prediction for first-in-human dosing was evaluated using allometric scaling, liver blood flow, and a fixed coefficient method, and single species allometric scaling using monkey data was most predictive for human pharmacokinetics of FXaI16L.

Published

2017

6. Evaluation of biomarkers for monitoring thrombogenic potential of FXaI16L

Author

Karrie A. Brenneman, Fei Hua, Kay A. Criswell, John E Graves, Michael W. Bolt, and Steven Arkin

Subjects

030204 cardiovascular system & hematology, Pharmacology, Fibrinogen, 03 medical and health sciences, Mice, 0302 clinical medicine, Tissue factor pathway inhibitor, Thrombin, medicine, Animals, Humans, Platelet, cardiovascular diseases, Rats, Wistar, Prothrombin time, medicine.diagnostic_test, business.industry, Antithrombin, Anticoagulants, Thrombosis, Hematology, General Medicine, Haplorhini, Rats, Factor Xa, cardiovascular system, Blood Coagulation Tests, business, Protein C, Biomarkers, circulatory and respiratory physiology, 030215 immunology, medicine.drug, Partial thromboplastin time

Abstract

A zymogen-like activated factor X variant (FXa) is being developed for treating acute bleeding conditions. Activated factor V is an essential cofactor to FXa for activating prothrombin to thrombin. Thrombi/emboli formation was observed microscopically in FXa toxicity studies in animals. The objective of this research was to evaluate candidate biomarkers for FXa-induced thrombi/emboli formation to inform safety monitoring and dose-escalation decisions in FXa clinical trials. Effects of intravenous FXa administration on platelets, fibrinogen, activated partial thromboplastin time (aPTT), prothrombin time (PT), D-dimer, tissue factor pathway inhibitor, thrombin : antithrombin complex, antithrombin, and factor V, and protein C (PC) activities were evaluated in mice, rats, and monkeys. Mice had endogenous factor V activity 10× that of monkeys and were overly sensitive to FXa-induced thrombi/emboli formation. In monkeys, decreases in fibrinogen and prolongation in aPTT and PT emerged as potential biomarkers for impending FXa-induced thrombi/emboli formation, based on association of changes with microscopically observable thrombi/emboli (0-97 thrombi/emboli per monkey). PC decreases, measured by a clot-based assay, were also observed. A similar reduction in PC activity, when measured by clot-based assay, was observed in a phase 1 clinical trial. However, an in-vitro experiment with human plasma spiked with increasing concentrations of FXa indicated dose-dependent FXa-induced interference with clot-based assays and no depletion of PC or S by FXa in non-clot-based assays. Nonclinical biomarker studies identified fibrinogen, aPTT and PT as potential biomarkers for monitoring the clinical safety of FXa. Results of clot-based assays with FXa treatment should be interpreted with caution.

Published

2019

7. Induction and Impact of Anti-Drug Responses Elicited by a Human Recombinant Coagulation Factor FXaI16L in Preclinical Species

Author

Rob Webster, Chuenlei Parng, Boris Gorovits, Debra D. Pittman, Michael W. Bolt, Lisa Dyleski, and Teresa M Caiazzo

Subjects

Drug, congenital, hereditary, and neonatal diseases and abnormalities, media_common.quotation_subject, Pharmaceutical Science, Pharmacology, 030226 pharmacology & pharmacy, law.invention, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, immune system diseases, law, Medicine, Neutralizing antibody, media_common, biology, business.industry, Immunogenicity, Antibody titer, nutritional and metabolic diseases, hemic and immune systems, enzymes and coenzymes (carbohydrates), Titer, 030220 oncology & carcinogenesis, Pharmacodynamics, biology.protein, Recombinant DNA, business

Abstract

This paper presents a systemic investigation of ADA development and ADA impact of a human coagulation factor in nonclinical species during drug development and provides insights into potential implications in human if a similar ADA occurs. FXaI16L-induced ADA response was characterized in monkey, mouse, rat, and dog in different studies, and ADA effects on pharmacokinetic and/or pharmacodynamics of FXaI16L were further examined in ADA-negative and ADA-positive animals. After repeated administrations, FXaI16L elicited a dose and exposure day-dependent ADA response which ranged from no response to a transient or persistent response. Increase in exposure day and increase in dose generally enhanced ADA incidence except for a decrease in ADA incidence was observed in monkeys after repeated high-dose administrations. The observable ADA impact on pharmacokinetics was only found in some ADA+ animals and included decrease in clearance and increase in systemic exposure but no increase in half-life. In addition, no or limited effect on pharmacodynamics by ADA was observed. The earliest ADA response was observed after three exposure days, marked elevation of drug exposure was observed in some animals at log titer > 2.0, and the highest antibody titer excited was about 4 (Log10) in all species. A correlation between ADA induction and accumulative exposure after various repeat treatments in different species was found for FXaI16L. In addition, potential immunogenicity risk and mitigation of ADA in clinics are discussed.

Published

2019

8. Nonclinical Evaluation of PF-06438179: A Potential Biosimilar to Remicade® (Infliximab)

Author

Leslie G. Lorello, Jim McNally, Hugh D. Conlon, Michael W. Leach, Carol F. Kirchhoff, Teresa Annette Smolarek, Andrew Saati, Sarah Koob, Mazin Derzi, Ahmed M. Shoieb, Penny Sharpe, Michael W. Bolt, and Theodore R. Johnson

Subjects

Monoclonal antibody, Male, 0301 basic medicine, Tumor necrosis factor, medicine.drug_class, Pharmacology toxicology, Drug Evaluation, Preclinical, Remicade, Pharmacology, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, medicine, Animals, Pharmacology (medical), Biosimilar Pharmaceuticals, Original Research, Medicine(all), 030203 arthritis & rheumatology, Toxicity, Tumor Necrosis Factor-alpha, business.industry, Biosimilar, Antibodies, Monoclonal, General Medicine, Infliximab, Toxicokinetics, Rats, Human tumor, Treatment Outcome, 030104 developmental biology, Liver, Immunology, Administration, Intravenous, Tumor necrosis factor alpha, business, Immunosuppressive Agents, medicine.drug

Abstract

Introduction PF-06438179, a potential biosimilar to Remicade® (infliximab, Janssen Biotech, Inc.), is a chimeric mouse–human monoclonal antibody targeting human tumor necrosis factor alpha (TNF). Methods Analytical (small subset reported here) and nonclinical studies compared the structural, functional, and in vivo nonclinical similarity of PF-06438179 with Remicade sourced from the United States (infliximab-US) and/or European Union (infliximab-EU). Results The peptide map profiles were superimposable, and peptide masses were the same, indicating identical amino acid sequences. Data on post-translational modifications, biochemical properties, and biological function provided strong support for analytical similarity. Administration of a single intravenous (IV) dose (10 or 50 mg/kg) of PF-06438179 or infliximab-EU to male rats was well tolerated. There were no test article-related clinical signs or effects on body weight or food consumption. Systemic exposures [maximum drug concentration (C max) and area under the concentration–time curve (AUC)] in rats administered PF-06438179 or infliximab-EU were similar, with mean exposure ratio of PF-06438179 relative to infliximab-EU ranging from 0.88 to 1.16. No rats developed anti-drug antibodies. A 2-week IV toxicity study was conducted with once-weekly administration of 10 or 50 mg/kg of PF-06438179 to male and female rats. PF-06438179-related hyperplasia of sinusoidal cells occurred in the liver in rats administered 50 mg/kg, but was not adverse based on its minimal to mild severity. The no-observed adverse-effect level for PF-06438179 was 50 mg/kg. At this dose, C max was 1360 µg/mL and AUC at 168 h was 115,000 µg h/mL on day 8. Conclusions The analytical and nonclinical studies have supported advancement of PF-06438179 into global comparative clinical trials. Funding Pfizer Inc.

Published

2016

9. Current nonclinical testing paradigm enables safe entry to First-In-Human clinical trials: The IQ consortium nonclinical to clinical translational database

Author

Thomas W. Jones, Timothy K. Hart, Maggie Liu, Michael W. Bolt, Donna Dambach, Vivek J. Kadambi, Douglas A. Keller, Thomas M. Monticello, and David M. Potter

Subjects

0301 basic medicine, Databases, Factual, Drug Industry, Drug-Related Side Effects and Adverse Reactions, Concordance, Drug Evaluation, Preclinical, Context (language use), Toxicology, computer.software_genre, Risk Assessment, Translational Research, Biomedical, 03 medical and health sciences, Medicine, Animals, Humans, Animal testing, Adverse effect, Pharmacology, Database, business.industry, Clinical trial, 030104 developmental biology, Drug development, Toxicity, Models, Animal, Animal studies, business, computer

Abstract

The contribution of animal testing in drug development has been widely debated and challenged. An industry-wide nonclinical to clinical translational database was created to determine how safety assessments in animal models translate to First-In-Human clinical risk. The blinded database was composed of 182 molecules and contained animal toxicology data coupled with clinical observations from phase I human studies. Animal and clinical data were categorized by organ system and correlations determined. The 2×2 contingency table (true positive, false positive, true negative, false negative) was used for statistical analysis. Sensitivity was 48% with a 43% positive predictive value (PPV). The nonhuman primate had the strongest performance in predicting adverse effects, especially for gastrointestinal and nervous system categories. When the same target organ was identified in both the rodent and nonrodent, the PPV increased. Specificity was 84% with an 86% negative predictive value (NPV). The beagle dog had the strongest performance in predicting an absence of clinical adverse effects. If no target organ toxicity was observed in either test species, the NPV increased. While nonclinical studies can demonstrate great value in the PPV for certain species and organ categories, the NPV was the stronger predictive performance measure across test species and target organs indicating that an absence of toxicity in animal studies strongly predicts a similar outcome in the clinic. These results support the current regulatory paradigm of animal testing in supporting safe entry to clinical trials and provide context for emerging alternate models.

Published

2017

10. Selective stalling of human translation through small-molecule engagement of the ribosome nascent chain

Author

David W. Piotrowski, Jennifer A. Doudna, Kim F. McClure, Spiros Liras, Michael W. Bolt, Bruce A. Maguire, Austin Huang, Robert Dullea, Donna N. Petersen, Jun Xiao, Tim Rolph, Liuqing Wei, Jamie H. D. Cate, Allyn T. Londregan, Kieran F. Geoghegan, Nathanael G. Lintner, Paula M. Loria, and Khosla, Chaitan

Subjects

0301 basic medicine, Proteomics, Male, Physiology, Gene Expression, Genetic Footprinting, Biochemistry, Medical and Health Sciences, Mass Spectrometry, 0302 clinical medicine, Heterocyclic Compounds, Medicine and Health Sciences, Ribosome profiling, Molecular Targeted Therapy, Biology (General), Spectrometric Identification of Proteins, General Neuroscience, Messenger RNA, Stable Isotope Labeling by Amino Acids in Cell Culture, Shine-Dalgarno sequence, Biological Sciences, Lipids, 3. Good health, Cell biology, Enzymes, Body Fluids, Nucleic acids, Blood, Cholesterol, T arm, Rabbits, Cellular Structures and Organelles, Anatomy, Proprotein Convertase 9, General Agricultural and Biological Sciences, Oxidoreductases, Luciferase, EF-Tu, Research Article, or More Rings, QH301-705.5, Genetic Fingerprinting and Footprinting, Biology, Research and Analysis Methods, General Biochemistry, Genetics and Molecular Biology, Blood Plasma, Cell Line, 03 medical and health sciences, Prokaryotic translation, Genetics, Escherichia coli, Initiation factor, Animals, Humans, Molecular Biology Techniques, Molecular Biology, General Immunology and Microbiology, Cell-Free System, Agricultural and Veterinary Sciences, Biology and Life Sciences, Proteins, Cell Biology, 4 or More Rings, Proprotein convertase, Rats, Internal ribosome entry site, 030104 developmental biology, Hela Cells, Protein Biosynthesis, Enzymology, RNA, Protein Translation, Sprague-Dawley, Ribosomes, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Proprotein convertase subtilisin/kexin type 9 (PCSK9) plays a key role in regulating the levels of plasma low-density lipoprotein cholesterol (LDL-C). Here, we demonstrate that the compound PF-06446846 inhibits translation of PCSK9 by inducing the ribosome to stall around codon 34, mediated by the sequence of the nascent chain within the exit tunnel. We further show that PF-06446846 reduces plasma PCSK9 and total cholesterol levels in rats following oral dosing. Using ribosome profiling, we demonstrate that PF-06446846 is highly selective for the inhibition of PCSK9 translation. The mechanism of action employed by PF-06446846 reveals a previously unexpected tunability of the human ribosome that allows small molecules to specifically block translation of individual transcripts., Author summary Many disease-mediating proteins have proven difficult to target with traditional small-molecule pharmaceuticals. In this paper, we report that a small molecule, PF-06446846, directly inhibits translation of one such protein, proprotein convertase subtilisin/kexin type 9 (PCSK9), by acting on the translating human ribosome. PF-06446846 causes the translating ribosome to stall soon after translating the PCSK9 signal sequence. We further show that PF-06446846 activity is dependent on the amino acid sequence of the nascent chain inside the ribosome exit tunnel. In a rat safety study, we observe decreases in plasma PCSK9, total cholesterol, and low-density lipoprotein (LDL) cholesterol. Using mass spectrometry in cell culture and ribosome profiling, we demonstrate that despite acting on the ribosome, which synthesizes every protein in the cell, PF-06446846 displays a high level of selectivity for PCSK9. This unexpected potential for small molecules to selectively inhibit the human ribosome opens the possibility for future development of small molecules targeting disease-mediating proteins that were previously thought to be undruggable.

Published

2017

11. The ‘totality-of-the-evidence’ approach in the development of PF-06438179/GP1111, an infliximab biosimilar, and in support of its use in all indications of the reference product

Author

Carol F. Kirchhoff, Joseph E. McClellan, Michael W. Bolt, Vatche Kalfayan, Muhammad I. Rehman, Rameshraja Palaparthy, and Hugh D. Conlon

Subjects

Oncology, medicine.medical_specialty, extrapolation, PF-06438179/GP1111, Review, Disease, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, totality of the evidence, medicine, Clinical efficacy, lcsh:RC799-869, Tumor necrosis factor binding, 030203 arthritis & rheumatology, business.industry, Gastroenterology, In vitro toxicology, Biosimilar, medicine.disease, Infliximab, Reference product, 030220 oncology & carcinogenesis, Rheumatoid arthritis, lcsh:Diseases of the digestive system. Gastroenterology, biosimilar, infliximab, business, medicine.drug

Abstract

The ‘totality-of-the-evidence’ biosimilarity concept requires that sufficient structural, functional, nonclinical, and clinical data are acquired in a stepwise manner, to demonstrate that no clinically meaningful differences in quality, safety, or efficacy are observed compared with the reference product. We describe the totality of the evidence for PF-06438179/GP1111 (PF-SZ-IFX; IXIFI™ [infliximab-qbtx]/Zessly®) that supported its approval as an infliximab (IFX) biosimilar for all eligible indications of reference IFX (ref-IFX; Remicade®) in Europe and in the US. Analytical similarity involving in vitro assays capable of distinguishing structural or functional differences between PF-SZ-IFX and ref-IFX formed a foundation for the biosimilarity exercise. Differences identified in N-glycosylation and charge heterogeneity were found not to impact the results in in vitro biological assays reflective of the pharmacology underlying the mechanisms of action (tumor necrosis factor binding, reverse signaling, antibody-dependent cell-mediated cytotoxicity and complement-dependent cytotoxicity) of IFX across disease indications. Similarity was assessed in a comparative clinical pharmacokinetic study and in a clinical efficacy and safety study in patients with rheumatoid arthritis, where therapeutic equivalence between PF-SZ-IFX and ref-IFX provided confirmatory evidence of biosimilarity, and, when coupled with the analytical similarity already established, supported extrapolation to all eligible disease indications of ref-IFX.

Published

2019

12. A compound that directly and selectively stalls PCSK9 translation

Author

Jun Xiao, Tim Rolph, Spiros Liras, David W. Piotrowski, Nathanael G. Lintner, Austin Huang, Robert Dullea, Allyn T. Londregan, Paula M. Loria, Bruce A. Maguire, Jamie H. D. Cate, Kieran F. Geoghegan, Liuqing Wei, Michael W. Bolt, Jennifer A. Doudna, Kim F. McClure, and Donna N. Petersen

Subjects

0303 health sciences, PCSK9, Subtilisin, Biology, Proprotein convertase, Ribosome, 3. Good health, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Mechanism of action, Biochemistry, medicine, Kexin, Initiation factor, Ribosome profiling, medicine.symptom, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Proprotein Convertase Subtilisin/Kexin Type 9 (PCSK9) plays a key role in regulating the levels of plasma low density lipoprotein cholesterol (LDL-C). Here we demonstrate that the compound PF-06446846 inhibits translation of PCSK9 by inducing the ribosome to stall around codon 34, mediated by the sequence of the nascent chain within the exit tunnel. We further show that PF-06446846 reduces plasma PCSK9 and total cholesterol levels in rats following oral dosing. Using ribosome profiling, we demonstrate that PF-06446846 is highly selective for the inhibition of PCSK9 translation. The mechanism of action employed by PF-06446846 reveals a previously unexpected tunability of the human ribosome, which allows small molecules to specifically block translation of individual transcripts.One Sentence SummaryA small-molecule PCSK9 inhibitor targets the human ribosome and selectively prevents PCSK9 synthesis.

Published

2016