Your search keyword '"Heather Myler"' showing total 39 results

1. Biological Matrix Supply Chain Shortages: More Matrices Are Now Rare—the Case for Surrogate Matrices

Author

Evan A, Dubiel, Heather, Myler, Mark E, Arnold, Patrick, Bennett, Jeff, Gatz, Elizabeth, Groeber, Seema, Gupta, Cheikh, Kane, Fumin, Li, William, Mylott, Courtney, Noah, Mark, O'Dell, Eric, Tewalt, Dominic, Warrino, and Andrew, Vick

Subjects

COVID-19, Humans, Pharmaceutical Science, Pandemics

Abstract

The COVID-19 pandemic has strained the biological matrix supply chain. An upsurge in demand driven by numerous COVID-19 therapeutic and vaccine development programs to combat the pandemic, along with logistical challenges sourcing and transporting matrix, has led to increased lead times for multiple matrices. Biological matrix shortages can potentially cause significant delays in drug development programs across the pharmaceutical and biotechnology industry. Given the current circumstances, discussion is warranted around what will likely be increased use of surrogate matrices in support of pharmacokinetic (PK), immunogenicity, and biomarker assays for regulatory filings. Regulatory authorities permit the use of surrogate matrix in bioanalytical methods in instances where matrix is rare or difficult to obtain, as long as the surrogate is appropriately selected and scientifically justified. Herein, the scientific justification and possible regulatory implications of employing surrogate matrix in PK, immunogenicity, and biomarker assays are discussed. In addition, the unique challenges that cell and gene therapy (CGT) and other innovative therapeutic modalities place on matrix supply chains are outlined. Matrix suppliers and contract research organizations (CROs) are actively implementing mitigation strategies to alleviate the current strain on the matrix supply chain and better prepare the industry for any future unexpected strains. To maintain ethical standards, these mitigation strategies include projecting matrix needs with suppliers at least 6 months in advance and writing or updating study protocols to allow for additional matrix draws from study subjects and/or re-purposing of subject matrix from one drug development program to another.

Published

2022

2. Evaluation of single molecule array digital immunoassay technology to quantitate neurofilament light chain

Author

Katie Matys, Alexa Broadnax, Patrick Bennett, Brittany Binion, Heather Myler, Krishna K Midde, Jake Harman, Mike Edwards, and Thomas Oglesby

Subjects

Bioanalysis, Neurofilament light, Clinical Biochemistry, Immunologic Tests, Bioinformatics, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Neurofilament Proteins, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Amyotrophic lateral sclerosis, 030304 developmental biology, Immunoassay, 0303 health sciences, Therapeutic regimen, medicine.diagnostic_test, business.industry, Ligand binding assay, Neurodegeneration, General Medicine, medicine.disease, Biomarker (cell), Medical Laboratory Technology, business, 030217 neurology & neurosurgery

Abstract

Aim: Globally, neurodegeneration accounts for significant morbidity and mortality among the elderly. Millions of people are afflicted with neurodegenerative diseases, with the most notable cases attributed to Alzheimer’s, Huntington’s, amyotrophic lateral sclerosis and Parkinson’s diseases. Sensitive assays that can detect proteopathic anomalies indicative of early neurodegeneration have remained elusive. Therefore, there is an urgent need for sensitive diagnostic and prognostic biomarker assays that can guide the therapeutic regimen in the clinic. Materials & methods: Single molecule array digital immunoassay platform has sensitivity about 1000-fold higher than traditional ligand binding assays. Consequently, we are now beginning to implement ultrasensitive techniques in bioanalysis. Conclusion: In the current study, we evaluated single molecule array technology and report specifications to quantitate neurofilament light chain, a bona-fide biomarker for neurodegeneration. Preliminary neurofilament light screening results from 100 human geriatric cerebrospinal fluid samples displayed huge biological variation and warrants further investigation.

Published

2020

3. Anti-drug Antibody Validation Testing and Reporting Harmonization

Author

Jim McNally, Szilárd Kamondi, Daniel Kramer, Honglue Shen, Vibha Jawa, Jane Ruppel, Charles S Hottenstein, Kelli R. Phillips, Meina Liang, Michael E Hodsdon, Dong Geng, Joanne Goodman, Mohsen Rajabi Ahbari, Heather Myler, Marta Starcevic Manning, Alvydas Mikulskis, William Hallett, Haoheng Yan, Adrienne Clements-Egan, Paul Chamberlain, Qiang Qu, ZhenZhen Liu, Carol Gleason, Viswanath Devanaryan, George R Gunn, Susan M. Richards, Theresa J Goletz, Troy E. Barger, Susana Liu, Lakshmi Amaravadi, Veerle Snoeck, Joao Pedras-Vasconcelos, Kathryn Lindley, Robert Nelson, Mark Ware, Shobha Purushothama, An Song, Susan Kirshner, Brian M Janelsins, Jad Zoghbi, Steven Bowen, and Ronald R. Bowsher

Subjects

Computer science, Sample processing, Pharmaceutical Science, Positive control, Harmonization, Sample (statistics), Assay sensitivity, Anti-Drug Antibody, Antibodies, United States, Sample stability, Validation testing, Europe, Risk analysis (engineering), Biological Assay

Abstract

Evolving immunogenicity assay performance expectations and a lack of harmonized anti-drug antibody validation testing and reporting tools have resulted in significant time spent by health authorities and sponsors on resolving filing queries. Following debate at the American Association of Pharmaceutical Sciences National Biotechnology Conference, a group was formed to address these gaps. Over the last 3 years, 44 members from 29 organizations (including 5 members from Europe and 10 members from FDA) discussed gaps in understanding immunogenicity assay requirements and have developed harmonization tools for use by industry scientists to facilitate filings to health authorities. Herein, this team provides testing and reporting strategies and tools for the following assessments: (1) pre-study validation cut point; (2) in-study cut points, including procedures for applying cut points to mixed populations; (3) system suitability control criteria for in-study plate acceptance; (4) assay sensitivity, including the selection of an appropriate low positive control; (5) specificity, including drug and target tolerance; (6) sample stability that reflects sample storage and handling conditions; (7) assay selectivity to matrix components, including hemolytic, lipemic, and disease state matrices; (8) domain specificity for multi-domain therapeutics; (9) and minimum required dilution and extraction-based sample processing for titer reporting. Graphical Abstract

Published

2021

4. AAPS Workshop Report on ICH M10

Author

Heather Myler, Faye Vazvaei, Eric Woolf, Eric Fluhler, and Brian Booth

Subjects

business.industry, 010401 analytical chemistry, Pharmacology toxicology, Pharmaceutical Science, Harmonization, Pharmacy, Public consultation, Guideline, Validation Studies as Topic, Meeting Report, 030226 pharmacology & pharmacy, 01 natural sciences, 0104 chemical sciences, 03 medical and health sciences, 0302 clinical medicine, Human use, Political science, Engineering ethics, business, Regional differences

Abstract

Over the last decade, several regulatory guidelines on bioanalytical method validation (BMV) have been issued by regulatory agencies around the world. This has left the bioanalytical community struggling with regional differences in regulatory expectations when preparing for global pharmaceutical submissions. The International Council for Harmonization of Technical Requirements for Pharmaceuticals for Human Use (ICH) has the mission to achieve greater harmonization worldwide to ensure that safe, effective, and high-quality medicines are developed and registered in the most resource-efficient manner. Following calls for harmonization, ICH-selected bioanalytical method validation and sample analysis among its topics for guidance development and earlier this year released a draft guideline (M10) on BMV for public consultation. In response, the American Association of Pharmaceutical Scientists (AAPS) held a 3-day workshop to provide a forum for regulatory, industry, and academic scientists to discuss the guideline and hear various points of view on key aspects. While there was agreement that the draft guideline is generally well written and comprehensive, specific topics generated considerable discussion and, in some cases, revision recommendations for consideration by the expert working group (EWG) responsible for the guideline content. This report provides a summary of the workshop proceedings.

Published

2019

5. Singlicate Ligand Binding Assay Using an Automated Microfluidic System: a Clinical Case Study

Author

Jonathan Haulenbeek, Kelli R. Phillips, Ross Fergus, Hao Jiang, Craig Titsch, Frank Zambito, Janice Gambardella, Heather Myler, Jennifer Cummings, and Alex Kozhich

Subjects

Accuracy and precision, Bioanalysis, Chromatography, medicine.drug_class, Chemistry, Coefficient of variation, Ligand binding assay, Microfluidics, 010401 analytical chemistry, Antibodies, Monoclonal, Pharmaceutical Science, Pharmacology, Ligands, Monoclonal antibody, 030226 pharmacology & pharmacy, 01 natural sciences, System a, 0104 chemical sciences, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Clinical case, Early phase

Abstract

The bioanalytical strategy for monoclonal antibody therapeutics, intended for multiple oncology indications, includes multiple integrated measurements of pharmacologically relevant therapeutics from discovery through development. Three ligand binding assays were cohesively developed and validated, as applicable, using the Gyrolab microfluidic system for the measurement of a free monoclonal antibody BMS-986207. Accuracy and precision demonstrate %bias from −6.3 to 4.4%, percent coefficient of variation (%CV) from 2.6 to 9.8%, and total error from 4.2 to 13.4% in the nonclinical assay; %bias from −0.3 to 3.3%, %CV from 3.5 to 18.2%, and total error from 6.1 to 19.7% in the clinical assay; and >97% of the sample meeting incurred sample reanalysis criteria. The clinical assay was validated using singlicate wells after gaining significant data in the early phase studies to support this cost-effective and efficient strategy. Each assay met fit-for-purpose and/or regulated bioanalytical method validation criteria including stability, selectivity, dilutional linearity, carryover, and specificity criteria with no interference from co-administered monoclonal antibody.

Published

2017

6. Perspectives on exploring hybrid LBA/LC-MS approach for clinical immunogenicity testing

Author

Jianing Zeng, Johanna R Mora, Hao Jiang, Renuka Pillutla, Heather Myler, and Gerry Kolaitis

Subjects

Drug, Bioanalysis, media_common.quotation_subject, Clinical Biochemistry, Computational biology, 030226 pharmacology & pharmacy, 01 natural sciences, Mass Spectrometry, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Drug tolerance, Liquid chromatography–mass spectrometry, Limit of Detection, Medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, media_common, business.industry, Immunogenicity, Ligand binding assay, 010401 analytical chemistry, General Medicine, Gold standard (test), 0104 chemical sciences, Social Control, Formal, Medical Laboratory Technology, Drug development, Immunologic Techniques, business, Artifacts, Chromatography, Liquid

Abstract

Biological drug products may elicit an antidrug antibody (ADA) response. The current widely used bridging ligand binding assay (LBA) is the gold standard for ADA assessments in drug development, which is a qualitative assay followed by a quasi-quantitative titer analysis but can be prone to interferences from biological matrices, drug targets and circulating drugs. We present our perspectives and findings in exploring a hybrid LBA/LC–MS as an orthogonal bioanalytical tool for clinical immunogenicity assessments. The hybrid LBA/LC–MS is a semiquantitative assay with acceptable specificity, drug tolerance and the capability of multiplexed detection of ADA isotypes. The assay results suggest this technology to be a promising and complementary bioanalytical tool that can provide informative immunogenicity data in drug development.

Published

2019

7. Report on the AAPS Immunogenicity Guidance Forum

Author

Adrienne Clements-Egan, Binodh DeSilva, Viswanath Devanarayan, Boris Gorovits, George R. Gunn, Vinod P. Shah, Kelli R. Phillips, Susan Kirshner, and Heather Myler

Subjects

medicine.medical_specialty, Pharmacology toxicology, Pharmaceutical Science, Guidelines as Topic, Pharmacy, 030226 pharmacology & pharmacy, Antibodies, Food and drug administration, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, Animals, Medicine, Medical physics, Pharmaceutical industry, Biological Products, United States Food and Drug Administration, business.industry, Immunogenicity, Proteins, Therapeutic protein, Assay sensitivity, United States, ComputingMethodologies_PATTERNRECOGNITION, 030220 oncology & carcinogenesis, business

Abstract

In September 2018, the American Association of Pharmaceutical Scientists (AAPS) conducted an Annual Guidance Forum on the considerations related to immunogenicity testing for therapeutic protein products. In addition to a broad representation by the pharmaceutical industry, the event included strong representation by leading scientists from the US Food and Drug Administration (FDA). The agency and industry perspectives and updates to the guidance were presented. Specific topics that were discussed included the strategies of anti-drug antibody (ADA) assay cut-point assessments, the selection of ADA-positive controls (PCs), and the evaluation of PC performance. Assessment strategies and relevance of ADA assay attributes were also discussed, including assay drug tolerance and ADA assay sensitivity. The following is a summary of the discussion.

Published

2019

8. Validation of an integrated series of ligand-binding assays for the quantitative determination of antibody–drug conjugates in biological matrices

Author

Vangipuram S. Rangan, Amy Manney, Mark Saewert, Ang Liu, Binodh DeSilva, Donna Dail, Jennifer Cummings, Renuka Pillutla, Alex Kozhich, Heather Myler, Chetana Rao, Jian Wang, and Brian K. Hoffpauir

Subjects

Quality Control, Bioanalysis, Accuracy and precision, Analyte, Antibody-drug conjugate, Immunoconjugates, Metabolite, Clinical Biochemistry, 030226 pharmacology & pharmacy, 01 natural sciences, Lignans, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, General Pharmacology, Toxicology and Pharmaceutics, Immunoassay, Chromatography, Ligand binding assay, 010401 analytical chemistry, Antibodies, Monoclonal, General Medicine, Assay sensitivity, 0104 chemical sciences, body regions, Medical Laboratory Technology, Pharmaceutical Preparations, chemistry, Half-Life, Conjugate

Abstract

Background: The bioanalytical strategy for antibody–drug conjugates (ADC) includes multiple integrated measurements of pharmacologically relevant ADC. Methods & results: Three ligand-binding assays were validated for the measurement of total antibody, active ADC and total ADC. Accuracy and precision demonstrate %bias from -8 to 14%, %CV from 3 to 11% and total error from 3 to 21%, with >98% samples meeting incurred sample reanalysis criteria. Each assay met stability, selectivity, dilutional integrity, carry over and specificity criteria with no interference from associated metabolite/impurity. Given the active ADC assay sensitivity to payload, active ADC was used to assess drug to antibody ratio. Discussion & conclusion: Implementation of a microfluidic automated platform enabled high throughput sample analysis of multiple analytes with minimal sample processing.

Published

2016

9. Pre-existing Antibody: Biotherapeutic Modality-Based Review

Author

Adrienne Clements-Egan, Boris Gorovits, Heather Myler, Laura Salazar-Fontana, Manoj Rajadhyaksha, Kun Peng, Mary Birchler, Shobha Purushothama, Crystal Sung, Meina Liang, and Li Xue

Subjects

0301 basic medicine, Drug, Glycan, media_common.quotation_subject, Pharmaceutical Science, Review Article, Epitope, 03 medical and health sciences, 0302 clinical medicine, Animals, Humans, Medicine, Adverse effect, Autoantibodies, media_common, Biological Products, Modality (human–computer interaction), biology, business.industry, Immunogenicity, Antibodies, Monoclonal, Biological Therapy, 030104 developmental biology, Pre-existing, 030220 oncology & carcinogenesis, Immunology, biology.protein, Antibody, business

Abstract

Pre-existing antibodies to biotherapeutic drugs have been detected in drug-naïve subjects for a variety of biotherapeutic modalities. Pre-existing antibodies are immunoglobulins that are either specific or cross-reacting with a protein or glycan epitopes on a biotherapeutic compound. Although the exact cause for pre-existing antibodies is often unknown, environmental exposures to non-human proteins, glycans, and structurally similar products are frequently proposed as factors. Clinical consequences of the pre-existing antibodies vary from an adverse effect on patient safety to no impact at all and remain highly dependent on the biotherapeutic drug modality and therapeutic indication. As such, pre-existing antibodies are viewed as an immunogenicity risk factor requiring a careful evaluation. Herein, the relationships between biotherapeutic modalities to the nature, prevalence, and clinical consequences of pre-existing antibodies are reviewed. Initial evidence for pre-existing antibody is often identified during anti-drug antibody (ADA) assay development. Other interfering factors known to cause false ADA positive signal, including circulating multimeric drug target, rheumatoid factors, and heterophilic antibodies, are discussed.

Published

2016

10. Concerted application of LC-MS and ligand binding assays to better understand exposure of a large molecule drug

Author

Snaehal Gadkari, Kristina D. Chadwick, Alicja Batog, Weifeng Xu, Renuka Pillutla, Jennifer Wheeler, Binodh DeSilva, Craig Titsch, Bonnie Wang, Heather Myler, Chris M. Thompson, James Stahl, Robert Dodge, Lauren Hippeli, Hao Jiang, Scott Willett, and Brent Yamamoto

Subjects

0301 basic medicine, Drug, Biodistribution, Bioanalysis, Pentamer, media_common.quotation_subject, Clinical Biochemistry, Ligands, 030226 pharmacology & pharmacy, Analytical Chemistry, law.invention, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, law, Liquid chromatography–mass spectrometry, Tandem Mass Spectrometry, Toxicity Tests, Animals, Humans, Amino Acid Sequence, General Pharmacology, Toxicology and Pharmaceutics, media_common, Chemistry, Ligand binding assay, General Medicine, Medical Laboratory Technology, 030104 developmental biology, Biochemistry, Pharmaceutical Preparations, Recombinant DNA, Biological Assay, Chromatography, Liquid

Abstract

Aim: A ligand-binding assay (LBA) was used to measure exposure of PRM-151, the recombinant form of human pentraxin-2 (PTX-2), a complex pentamer with multiple binding partners. However, the assay showed a lack of dose-dependent exposure in select preclinical species and it could not differentiate the infused PRM-151 from the endogenous PTX-2 in nonhuman primates. Materials & methods: Instead of assessing interference from its multiple binding partners, which could be time consuming and laborious, a LC–MS assay avoid of these interference was implemented to measure ‘total’ drug without the use of immunoaffinity capture reagents. Results & Conclusion: The resultant LC–MS data confirmed the original data and the lack of dose-dependent exposure is now understood to be due to the multiple and diverse targets and functions and resultant complex biodistribution rather than an assay artifact.

Published

2018

11. Generic Anti-PEG Antibody Assay on ProterixBio's (Formerly BioScale) ViBE Platform Shows Poor Reproducibility

Author

Julie Shields, Heather Myler, Shannon D Chilewski, and Johanna R Mora

Subjects

Reproducibility, Chromatography, biology, Chemistry, Immunogenicity, Chemistry, Pharmaceutical, Pharmacology toxicology, Pharmaceutical Science, Reproducibility of Results, Enzyme-Linked Immunosorbent Assay, 030226 pharmacology & pharmacy, Method development, Antibodies, Polyethylene Glycols, 03 medical and health sciences, 0302 clinical medicine, Limit of Detection, 030220 oncology & carcinogenesis, PEG ratio, PEGylation, biology.protein, Humans, Microparticle, Antibody

Abstract

PEGylation is a modification commonly used to increase the half-life of therapeutic proteins. The strategy for immunogenicity testing of these compounds should include methods to detect both anti-protein and anti-PEG antibodies. We previously reported a method for the detection of anti-PEG antibodies using ProterixBio's (formerly BioScale) acoustic membrane microparticle (AMMP) technology. Our initial method development work showed the assay was capable of detecting antibodies in human serum with a sensitivity of 1 μg/mL with good reproducibility (CV 7%). Since the publication of this initial paper, additional experimentation was performed in an effort to validate the assay for support of clinical sample analysis. This additional data indicate that the method has high variability (CV% 20) and is unsuitable to support clinical sample analysis.

Published

2017

12. Development and characterization of antibody reagents to assess anti-PEG IgG antibodies in clinical samples

Author

Heather Myler, Martin J. Corbett, Steven P. Piccoli, Robert Dodge, Holly Palme, Zheng Lin, Jia Duo, Renuka Pillutla, Murli Krishna, and Binodh DeSilva

Subjects

Clinical Biochemistry, macromolecular substances, Polyethylene glycol, Conjugated system, Polyethylene Glycols, Analytical Chemistry, Mice, chemistry.chemical_compound, PEG ratio, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, Surface plasmon resonance, biology, Chemistry, Immunogenicity, technology, industry, and agriculture, General Medicine, Molecular biology, Antibodies, Anti-Idiotypic, Medical Laboratory Technology, Reagent, Antibody Formation, biology.protein, Antibody, Antibody formation

Abstract

Background: Polyethylene glycol (PEG) is a polymer that can be conjugated with therapeutic proteins. Monitoring anti-PEG antibodies in human subjects may be required as part of immunogenicity assessment. The lack of well-characterized anti-PEG reagents have limited our understanding of anti-PEG humoral response. Results: Antibodies reactive to PEG were engineered with a human IgG1 Fc. Surface plasmon resonance and plate-based methods demonstrated that their binding was dependent on molecular weight (MW) of PEG. Specificity experiments using chemical analogs identified their specificity. Conclusion: Affinity, specificity and MW of PEG are critical characteristics that impact interactions of anti-PEG antibodies with PEG. These attributes especially MW of PEG and the assay formats may impact the ability to detect anti-PEG antibodies.

Published

2015

13. The pharmacokinetics of peginterferon lambda-1a following single dose administration to subjects with impaired renal function

Author

Robert Adamczyk, Heather Myler, Michael Hesney, Michele Stonier, Elizabeth Colston, Richard Bertz, and Matthew Hruska

Subjects

Pharmacology, Volume of distribution, medicine.medical_specialty, Peginterferon lambda-1a, business.industry, Urology, Cmax, Renal function, Confidence interval, Surgery, Pharmacokinetics, Tolerability, Medicine, Pharmacology (medical), Geometric mean, business

Abstract

Aims This open label study was conducted to assess the effect of renal impairment (RI) on the pharmacokinetics (PK) of peginterferon lambda-1a (Lambda). Methods Subjects (age 18–75 years, BMI 18–35 kg m–2) were enrolled into one of five renal function groups: normal (n = 12), mild RI (n = 8), moderate RI (n = 8), severe RI (n = 7), end-stage renal disease (ESRD, n = 8) based on estimated glomerular filtration rate (eGFR) calculated using the Modification of Diet in Renal Disease (MDRD) equation. Subjects received a single dose of Lambda (180 µg) subcutaneously on day 1 followed by PK serum sample collections through day 29. Safety, tolerability and immunogenicity data were collected through day 43. PK parameters were estimated and summarized by group. Geometric mean ratios (GMR) and 90% confidence intervals (CIs) were calculated between normal and RI groups. Results With decreasing eGFR, Lambda exposure (Cmax, AUC) increased while apparent clearance (CL/F) and apparent volume of distribution (V/F) decreased. Relative to subjects with normal renal function (geometric mean AUC = 99.5 ng ml–1 h), Lambda exposure estimates (AUC) were slightly increased in the mild RI group (geometric mean [90% CI]: 1.20 [0.82, 1.77]) and greater in the moderate (1.95 [1.35, 2.83]), severe RI (1.95 [1.30, 2.93]) and ESRD (1.88 [1.30, 2.73]) groups. Lambda was generally well tolerated. Conclusions The results demonstrated that RI reduces the clearance of Lambda and suggests that dose modifications may not be required in patients with mild RI but may be required in patients with moderate to severe RI or ESRD.

Published

2015

14. An integrated multiplatform bioanalytical strategy for antibody–drug conjugates: a novel case study

Author

Jian Wang, Mei-Chen Sung, Binodh DeSilva, Robert Neely, Jennifer Cummings, Donna Dail, Steven P. Piccoli, John Lute, Heather Myler, Alexander T. Kozhich, Richard L. Wong, Thomas D. Kempe, Wendy Freebern, Anne-Françoise Aubry, Renuka Pillutla, Heather E. Vezina, Mark E. Arnold, Vangipuram S. Rangan, Mark Saewert, Bonnie Wang, Frank Zambito, David Passmore, Amy Manney, Shrikant Deshpande, Huidong Gu, and Ang Liu

Subjects

Drug, Bioanalysis, Immunoconjugates, biology, Computer science, media_common.quotation_subject, Clinical Biochemistry, Payload (computing), technology, industry, and agriculture, Antibodies, Monoclonal, Context (language use), Nanotechnology, General Medicine, Computational biology, Analytical Chemistry, Microtubule polymerization, body regions, Medical Laboratory Technology, biology.protein, Humans, Cleavable linker, General Pharmacology, Toxicology and Pharmaceutics, Antibody, media_common, Conjugate

Abstract

Background: The bioanalytical strategy for antibody–drug conjugates (ADC) includes numerous measurements integrally designed to provide comprehensive characterization of PK, PD and immunogenicity. This manuscript describes the utilization of reagents specifically tailored to an ADC with a microtubule polymerization inhibitor payload and cathepsin B cleavable linker. Methods: The PK strategy includes the evaluation of physiological levels of total antibody, active ADC, total ADC, antibody-conjugated payload and unconjugated payload. These data are evaluated in the context of target and antidrug antibody levels to elucidate bioactive ADC. Results & conclusion: Herein, we discuss how this strategy has been applied and present our preliminary observations. Continuously evolving to meet pipeline demands, the integrated bioanalytical data will provide critical insights into the exposure–response relationship.

Published

2015

15. 2014 White Paper on recent issues in bioanalysis: a full immersion in bioanalysis (Part 2 – hybrid LBA/LCMS, ELN & regulatory agencies’ input)

Author

Surinder Kaur, Swati Gupta, Eric Fluhler, John Smeraglia, Annik Bergeron, Mark E. Arnold, Timothy V Olah, Steven J. Swanson, Adrien Musuku, Lauren Stevenson, Olivier Le Blaye, Boris Gorovits, Ann Levesque, Fabio Garofolo, Gary Schultz, Mark J. Rose, Eric Woolf, Chris Beaver, Anne-Françoise Aubry, Li Xue, Heather Myler, Jason Wakelin-Smith, Mark Bustard, Hendrik Neubert, Dawn Dufield, Stacy Ho, Akiko Ishii-Watabe, Tong-Yuan Yang, Stephen C. Alley, Matthew Szapacs, Laura Cojocaru, Surendra Bansal, Keyang Xu, Shefali Patel, Faye Vazvaei, Mark Ma, Benno Ingelse, Emma Whale, Amanda Wilson, Roger Hayes, Sam Haidar, Binodh DeSilva, Noriko Katori, Lakshmi Amaravadi, Lindsay King, Isabelle Dumont, Xiao-Yan Cai, Jeff Duggan, Albert Torri, Steve Lowes, Leo Kirkovsky, and Jan Welink

Subjects

Bioanalysis, Engineering, Clinical Laboratory Techniques, business.industry, Clinical Biochemistry, Scientific excellence, Analytic Sample Preparation Methods, Nanotechnology, General Medicine, Mass Spectrometry, Analytical Chemistry, Medical Laboratory Technology, White paper, Humans, Engineering ethics, General Pharmacology, Toxicology and Pharmaceutics, business, Chromatography, Liquid

Abstract

The 2014 8th Workshop on Recent Issues in Bioanalysis (8th WRIB), a 5-day full immersion in the evolving field of bioanalysis, took place in Universal City, California, USA. Close to 500 professionals from pharmaceutical and biopharmaceutical companies, contract research organizations and regulatory agencies worldwide convened to share, review, discuss and agree on approaches to address current issues of interest in bioanalysis. The topics covered included both small and large molecules, and involved LCMS, hybrid LBA/LCMS, LBA approaches and immunogenicity. From the prolific discussions held during the workshop, specific recommendations are presented in this 2014 White Paper. As with the previous years’ editions, this paper acts as a practical tool to help the bioanalytical community continue advances in scientific excellence, improved quality and better regulatory compliance. Due to its length, the 2014 edition of this comprehensive White Paper has been divided into three parts for editorial reasons. This publication (Part 2) covers the recommendations for Hybrid LBA/LCMS, Electronic Laboratory Notebook and Regulatory Agencies’ Input. Part 1 (Small molecules bioanalysis using LCMS) was published in the Bioanalysis issue 6(22) and Part 3 (Large molecules bioanalysis using LBA and Immunogenicity) will be published in the Bioanalysis issue 6(24).

Published

2014

16. 2014 White Paper on recent issues in bioanalysis: a full immersion in bioanalysis (Part 3 – LBA and immunogenicity)

Author

Alison Joyce, Theingi M. Thway, Lakshmi Amaravadi, Laura Cojocaru, Faye Vazvaei, Mark Ma, Amanda Wilson, Albert Torri, Lauren Stevenson, Steven J. Swanson, Chris Beaver, Heather Myler, Isabelle Dumont, Annik Bergeron, Surendra Bansal, Benno Ingelse, Eric Fluhler, Susan Kirshner, Corinne Petit-Frere, Jason Wakelin-Smith, Boris Gorovits, Xiao-Yan Cai, Roger Hayes, Mark J. Rose, Eric Woolf, Renuka Pillutla, Ann Levesque, Omar F Laterza, Stephanie Fraser, Li Xue, Laura Salazar-Fontana, Lindsay King, Gary Schultz, Sheldon Leung, Tong-Yuan Yang, John Smeraglia, Sam Haidar, Stephen C. Alley, Dominique Gouty, Fabio Garofolo, Akiko Ishii-Watabe, Binodh DeSilva, Surinder Kaur, and Swati Gupta

Subjects

Medical Laboratory Technology, Bioanalysis, White paper, Political science, Clinical Biochemistry, Scientific excellence, Engineering ethics, Nanotechnology, General Medicine, General Pharmacology, Toxicology and Pharmaceutics, Analytical Chemistry

Abstract

The 2014 8th Workshop on Recent Issues in Bioanalysis (8th WRIB), a 5-day full immersion in the evolving field of bioanalysis, took place in Universal City, California, USA. Close to 500 professionals from pharmaceutical and biopharmaceutical companies, contract research organizations and regulatory agencies worldwide convened to share, review, discuss and agree on approaches to address current issues of interest in bioanalysis. The topics covered included both small and large molecules, and involved LCMS, hybrid LBA/LCMS, LBA approaches and immunogenicity. From the prolific discussions held during the workshop, specific recommendations are presented in this 2014 White Paper. As with the previous years’ editions, this paper acts as a practical tool to help the bioanalytical community continue advances in scientific excellence, improved quality and better regulatory compliance. Due to its length, the 2014 edition of this comprehensive White Paper has been divided into three parts for editorial reasons. This publication (Part 3) covers the recommendations for Large molecules bioanalysis using LBA and Immunogenicity. Part 1 (Small molecules bioanalysis using LCMS) and Part 2 (Hybrid LBA/LCMS, Electronic Laboratory Notebook and Regulatory Agencies' Input) were published in the Bioanalysis issues 6(22) and 6(23), respectively.

Published

2014

17. 2014 White Paper on recent issues in bioanalysis: a full immersion in bioanalysis (Part 1 – small molecules by LCMS)

Author

Li Xue, Mark J. Rose, Eric Woolf, Lauren Stevenson, Tong-Yuan Yang, Ann Lévesque, Olivier Le Blaye, Annik Bergeron, Jian Wang, Laura Cojocaru, Mark E. Arnold, Mark Bustard, Josée Michon, Daksha Desai-Krieger, Neil Spooner, John Smeraglia, Mary Carbone, Benno Ingelse, Eric Fluhler, Heather Myler, Jan Welink, Ronald Bauer, Tom Verhaeghe, Adrien Musuku, Faye Vazvaei, Fabio Garofolo, Isabelle Dumont, Jason Wakelin-Smith, Shefali Patel, Gary Schultz, Xiao-Yan Cai, Noriko Katori, Sam Haidar, Mark Ma, Emma Whale, Amanda Wilson, Timothy V Olah, Roger Hayes, Bruce Stouffer, Jeff Duggan, Steve Lowes, Katalina Mettke, Surendra Bansal, and Stacy Ho

Subjects

Validation study, Engineering, Bioanalysis, business.industry, Clinical Biochemistry, Scientific excellence, Nanotechnology, General Medicine, Analytical Chemistry, Medical Laboratory Technology, White paper, Engineering ethics, General Pharmacology, Toxicology and Pharmaceutics, business

Abstract

The 2014 8th Workshop on Recent Issues in Bioanalysis (8th WRIB), a 5-day full immersion in the evolving field of bioanalysis, took place in Universal City, California, USA. Close to 500 professionals from pharmaceutical and biopharmaceutical companies, contract research organizations and regulatory agencies worldwide convened to share, review, discuss and agree on approaches to address current issues of interest in bioanalysis. The topics covered included both small and large molecules, and involved LCMS, hybrid LBA/LCMS, LBA approaches and immunogenicity. From the prolific discussions held during the workshop, specific recommendations are presented in this 2014 White Paper. As with the previous years’ editions, this paper acts as a practical tool to help the bioanalytical community continue advances in scientific excellence, improved quality and better regulatory compliance. Due to its length, the 2014 edition of this comprehensive White Paper has been divided into three parts for editorial reasons. This publication (Part 1) covers the recommendations for small molecule bioanalysis using LCMS. Part 2 (Hybrid LBA/LCMS, Electronic Laboratory Notebook and Regulatory Agencies’ input) and Part 3 (Large molecules bioanalysis using LBA and Immunogenicity) will be published in the upcoming issues of Bioanalysis.

Published

2014

18. Measuring biotherapeutics with endogenous counterparts and pre-existing antibodies: an interferon case study

Author

Jie Zhu, Heather Myler, Tonya Felix, Matt Hruska, and Steven P. Piccoli

Subjects

Clinical Biochemistry, Endogeny, Reference laboratory, Analytical Chemistry, Assay interference, Pharmacokinetics, Interferon, Humans, Medicine, General Pharmacology, Toxicology and Pharmaceutics, Immunoassay, Serum pool, biology, business.industry, Interleukins, Antibodies, Monoclonal, Reproducibility of Results, General Medicine, Clinical trial, Medical Laboratory Technology, Immunology, biology.protein, Interferons, Antibody, business, medicine.drug

Abstract

Background: This article presents case study data demonstrating the importance of having a thorough understanding of matrix-interference in support of global clinical trials. Methods/Results: A ligand-binding assay used in the measurement of interferon lambda in human serum was transferred from the reference laboratory to a US-based comparator laboratory and then to a China-based comparator laboratory. The method was successfully validated at each laboratory, however, during cross-validation, there were notable differences, including 30–60% difference in incurred study sample results. The differences were attributed to matrix factors included in the serum pool used to prepare standards and quality controls. Newly procured serum (n = 75 individuals) was tested for assay interference. 12% contained either pre-existing antibodies (auto-antibodies) or were identified as pharmacokinetic assay outliers. Conclusion: Prescreening of serum to exclude reactive individuals resulted in successful cross-validation and the establishment of a high integrity pharmacokinetic assay in support of global clinical trials.

Published

2014

19. A White Paper—Consensus and Recommendations of a Global Harmonization Team on Assessing the Impact of Immunogenicity on Pharmacokinetic Measurements

Author

Jeffrey Sailstad, Heather Myler, Boris Gorovits, Adrienne Clements-Egan, J. T. Wustner, M. Putman, Lakshmi Amaravadi, Renuka Pillutla, M. K. Rose, L. Tang, S. Pursuhothama, and K. Sonehara

Subjects

Drug, medicine.medical_specialty, Consensus, media_common.quotation_subject, Risk-based testing, White Paper, Pharmaceutical Science, Harmonization, Pharmacology, White paper, Drug Therapy, Pharmacokinetics, Allergy and Immunology, Animals, Humans, Medicine, Medical physics, Antibodies, Blocking, media_common, business.industry, Immunogenicity, Legislation, Drug, Pharmacodynamics, business, Clearance

Abstract

The Global Bioanalysis Consortium (GBC) set up an international team to explore the impact of immunogenicity on pharmacokinetic (PK) assessments. The intent of this paper is to define the field and propose best practices when developing PK assays for biotherapeutics. We focus on the impact of anti-drug antibodies (ADA) on the performance of PK assay leading to the impact on the reported drug concentration and exposure. The manuscript describes strategies to assess whether the observed change in the drug concentration is due to the ADA impact on drug clearance rates or is a consequence of ADA interference in the bioanalytical method applied to measure drug concentration. This paper provides the bioanalytical scientist guidance for developing ADA-tolerant PK methods. It is essential that the data generated in the PK, ADA, pharmacodynamic and efficacy/toxicity evaluations are viewed together. Therefore, the extent for the investigation of the PK sensitivity to the presence of ADA should be driven by the project needs and risk based.

Published

2014

20. 2013 White Paper on recent issues in bioanalysis: ‘hybrid’ – the best of LBA and LCMS

Author

Sam Haidar, Stacy Ho, Lauren Stevenson, Surinder Kaur, Jeff Duggan, Alvydas Mikulskis, Jian Wang, Judy Shih, Magnus Knutsson, Lakshmi Amaravadi, Boris Gorovits, Rand Jenkins, Steve Lowes, Hanlan Liu, Mark Ma, Binodh DeSilva, Ronald Shoup, Emma Whale, Chad Ray, Christopher P. Evans, Marian Kelley, Jean W. Lee, An Song, João Tavares Neto, Bob Nicholson, Laixin Wang, Dominique Gouty, Rafiq Islam, Suzanne Martinez, Mike Losauro, Isabelle Dumont, Adrien Musuku, Dawn Dufield, Vincenzo Pucci, Shefali Patel, Eric Ormsby, Laura Wright, Margarete Brudny-Kloeppel, Valerie Theobald, Gary Schultz, Stephanie Fraser, Timothy V Olah, Noriko Katori, Richard Houghton, Mark E. Arnold, Eric Fluhler, Catherine Dicaire, Eric Woolf, Sherri Dudal, Fabio Garofolo, Jan Welink, Mario Rocci, Laurence Mayrand-Provencher, Heather Myler, Raymond Naxing Xu, Jason Wakelin-Smith, Brian Booth, Roger Hayes, Craig Simon, Surendra Bansal, and Theingi M. Thway

Subjects

Medical Laboratory Technology, Bioanalysis, White paper, Political science, Clinical Biochemistry, Nanotechnology, Engineering ethics, General Medicine, Validation Studies as Topic, General Pharmacology, Toxicology and Pharmaceutics, Analytical Chemistry

Abstract

The 2013 7th Workshop on Recent Issues in Bioanalysis was held in Long Beach, California, USA, where close to 500 professionals from pharmaceutical and biopharmaceutical companies, CROs and regulatory agencies convened to discuss current topics of interest in bioanalysis. These ‘hot’ topics, which covered both small and large molecules, were the starting point for fruitful exchanges of knowledge, and sharing of ideas among speakers, panelists and attendees. The discussions led to specific recommendations pertinent to bioanalytical science. Such as the previous editions, this 2013 White Paper addresses important bioanalytical issues and provides practical answers to the topics presented, discussed and agreed upon by the global bioanalytical community attending the 7th Workshop on Recent Issues in Bioanalysis.

Published

2013

21. Tiered approach to anti-drug antibody testing

Author

Heather Myler and Robert Dodge

Subjects

business.industry, Immunology, Medicine, business, Tiered approach, Anti-Drug Antibody

Published

2013

22. A randomized, controlled study of peginterferon lambda-1a/ribavirin ± daclatasvir for hepatitis C virus genotype 2 or 3

Author

Megan Wind-Rotolo, Adrián Gadano, Christophe Hézode, Yukiko Inada, Joji Toyota, Anna Linda Zignego, Simone I. Strasser, Giovanni Battista Gaeta, Subasree Srinivasan, Jeong Heo, Simon Portsmouth, Sheng-Nan Lu, Patrick Marcellin, Wan-Long Chuang, Heather Myler, Seung Woon Paik, David Cohen, Christophe Moreno, Hiromitsu Kumada, Alexander J. Thompson, Matthew Hruska, Graham R. Foster, Fiona McPhee, Martti Färkkilä, Hugo Fainboim, Stuart K. Roberts, Kazuaki Chayama, John M. Vierling, Foster, Graham R., Chayama, Kazuaki, Chuang, Wan Long, Fainboim, Hugo, Farkkila, Martti, Gadano, Adrian, Gaeta, Giovanni Battista, Hézode, Christophe, Inada, Yukiko, Heo, Jeong, Kumada, Hiromitsu, Lu, Sheng Nan, Marcellin, Patrick, Moreno, Christophe, Roberts, Stuart K., Strasser, Simone I., Thompson, Alexander J., Toyota, Joji, Paik, Seung Woon, Vierling, John M., Zignego, Anna L., Cohen, David, Mcphee, Fiona, Wind Rotolo, Megan, Srinivasan, Subasree, Hruska, Matthew, Myler, Heather, Portsmouth, Simon D., Clinicum, Department of Medicine, and Gastroenterologian yksikkö

Subjects

0301 basic medicine, medicine.medical_specialty, Daclatasvir, Hepatitis C virus, Peginterferon alfa-2a, Population, Peginterferon-alfa, medicine.disease_cause, THERAPY, Gastroenterology, HCV GENOTYPE-2, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, INFECTION, Genotype, medicine, PLUS SOFOSBUVIR, education, CIRRHOSIS, education.field_of_study, Multidisciplinary, business.industry, Research, Ribavirin, Peginterferon lambda-1a, virus diseases, Genotype 2, Genotype 3, Virology, digestive system diseases, 3. Good health, 030104 developmental biology, chemistry, Tolerability, 3121 General medicine, internal medicine and other clinical medicine, Technologie de la sécurité, 030211 gastroenterology & hepatology, RIBAVIRIN, Hepatitis C viru, business, medicine.drug

Abstract

Background and purpose: Peginterferon Lambda was being developed as an alternative to alfa interferon for the treatment of chronic hepatitis C virus (HCV) infection. We compared peginterferon Lambda-1a plus ribavirin (Lambda/RBV) and Lambda/RBV plus daclatasvir (DCV; pangenotypic NS5A inhibitor) with peginterferon alfa-2a plus RBV (alfa/RBV) in treatment-naive patients with HCV genotype 2 or 3 infection. Methods: In this multicenter, double-blind, phase 3 randomized controlled trial, patients were assigned 2:2:1 to receive 24 weeks of Lambda/RBV, 12 weeks of Lambda/RBV + DCV, or 24 weeks of alfa/RBV. The primary outcome measure was sustained virologic response at post-treatment Week 12 (SVR12). Results: Overall, 874 patients were treated: Lambda/RBV, n = 353; Lambda/RBV + DCV, n = 349; alfa/RBV, n = 172. Patients were 65 % white and 33 % Asian, 57 % male, with a mean age of 47 years; 52 % were infected with genotype 2 (6 % cirrhotic) and 48 % with genotype 3 (9 % cirrhotic). In the Lambda/RBV + DCV group, 83 % (95 % confidence interval [CI] 78.5, 86.5) achieved SVR12 (90 % genotype 2, 75 % genotype 3) whereas SVR12 was achieved by 68 % (95 % CI 63.1, 72.9) with Lambda/RBV (72 % genotype 2, 64 % genotype 3) and 73 % (95 % CI 66.6, 79.9) with peginterferon alfa/RBV (74 % genotype 2, 73 % genotype 3). Lambda/RBV + DCV was associated with lower incidences of flu-like symptoms, hematological abnormalities, and discontinuations due to adverse events compared with alfa/RBV. Conclusion: The 12-week regimen of Lambda/RBV + DCV was superior to peginterferon alfa/RBV in the combined population of treatment-naive patients with genotype 2 or 3 infection, with an improved tolerability and safety profile compared with alfa/RBV., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2016

23. FGF21 Analogs of Sustained Action Enabled by Orthogonal Biosynthesis Demonstrate Enhanced Antidiabetic Pharmacology in Rodents

Author

Bruce E. Kimmel, Richard D. DiMarchi, Joel Berger, Anthony Manibusan, Zhihua Li, Qing Dallas-Yang, Margaret Wu, Dennis M. Zaller, Stuart Bussell, Jun Yao, Heather Myler, Anna-Maria A. Hays Putnam, James Mu, Nina Li, Bei B. Zhang, Thea Norman, Douglas W. Axelrod, Carlos G. Rodriguez, Jason Pinkstaff, Joseph M. Metzger, Darin Lee, and Lillian Skidmore

Subjects

Male, FGF21, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Adipose tissue, Biology, Pharmacology, Polyethylene Glycols, Rats, Sprague-Dawley, Mice, Insulin resistance, Internal Medicine, medicine, Animals, Humans, Hypoglycemic Agents, Protein kinase B, geography, geography.geographical_feature_category, Insulin, Body Weight, Islet, medicine.disease, Pharmacology and Therapeutics, Rats, Fibroblast Growth Factors, HEK293 Cells, Delayed-Action Preparations, PEGylation, Phosphorylation, Insulin Resistance, Energy Metabolism

Abstract

Fibroblast growth factor 21 (FGF21) mitigates many of the pathogenic features of type 2 diabetes, despite a short circulating half-life. PEGylation is a proven approach to prolonging the duration of action while enhancing biophysical solubility and stability. However, in the absence of a specific protein PEGylation site, chemical conjugation is inherently heterogeneous and commonly leads to dramatic loss in bioactivity. This work illustrates a novel means of specific PEGylation, producing FGF21 analogs with high specific activity and salutary biological activities. Using homology modeling and structure-based design, specific sites were chosen in human FGF21 for site-specific PEGylation to ensure that receptor binding regions were preserved. The in vitro activity of the PEGylated FGF21 ana-logs corresponded with the site of PEG placement within the binding model. Site-specific PEGylated analogs demonstrated dramatically increased circulating half-life and enhanced efficacy in db/db mice. Twice-weekly dosing of an optimal FGF21 analog reduced blood glucose, plasma lipids, liver triglycerides, and plasma glucagon and enhanced pancreatic insulin content, islet number, and glucose-dependent insulin secretion. Restoration of insulin sensitivity was demonstrated by the enhanced ability of insulin to induce Akt/protein kinase B phosphorylation in liver, muscle, and adipose tissues. PEGylation of human FGF21 at a specific and preferred site confers superior metabolic pharmacology.

Published

2012

24. 2015 White Paper on recent issues in bioanalysis: focus on new technologies and biomarkers (Part 3--LBA, biomarkers and immunogenicity)

Author

Daniel T. Mytych, Stephanie Fraser, Andre Nogueira da Costa, An Song, Michael Skelly, Susan Kirshner, John Smeraglia, Alyssa Morimoto, Soma Ray, Jeffrey Spond, Boris Gorovits, Corinna Krinos-Fiorotti, Natasha Savoie, Laura Salazar-Fontana, Afshin Safavi, Theingi M. Thway, Mark Ma, John Kamerud, Apollon Papadimitriou, Noriko Katori, Tong-Yuan Yang, Roland F Staack, Shannon D Chilewski, Herbert Birnboeck, Nilufer Tampal, Jad Zoghbi, Clare Kingsley, John Allinson, Marianne Scheel Fjording, Troy E. Barger, Renuka Pillutla, Rafiq Islam, Birgit Jaitner, Jan Welink, Sam Haidar, Susan M. Richards, Judy Shih, Martin Schaefer, Jim McNally, David Lanham, Viswanath Devanarayan, Bruce Stouffer, Shalini Gupta, Heather Myler, Linlin Luo, Yan G. Ni, Albert Torri, Lakshmi Amaravadi, and Fabio Garofolo

Subjects

Engineering, Bioanalysis, Emerging technologies, business.industry, Clinical Biochemistry, Scientific excellence, General Medicine, Antibodies, Neutralizing, Analytical Chemistry, Biotechnology, Biopharmaceutics, Medical Laboratory Technology, Biopharmaceutical, White paper, Humans, Engineering ethics, Biological Assay, General Pharmacology, Toxicology and Pharmaceutics, business, Biomarkers

Abstract

The 2015 9th Workshop on Recent Issues in Bioanalysis (9th WRIB) took place in Miami, Florida with participation of 600 professionals from pharmaceutical and biopharmaceutical companies, biotechnology companies, contract research organizations and regulatory agencies worldwide. WRIB was once again a 5 day, week-long event – A Full Immersion Bioanalytical Week – specifically designed to facilitate sharing, reviewing, discussing and agreeing on approaches to address the most current issues of interest in bioanalysis. The topics covered included both small and large molecules, and involved LCMS, hybrid LBA/LCMS and LBA approaches, including the focus on biomarkers and immunogenicity. This 2015 White Paper encompasses recommendations emerging from the extensive discussions held during the workshop, and is aimed to provide the bioanalytical community with key information and practical solutions on topics and issues addressed, in an effort to enable advances in scientific excellence, improved quality and better regulatory compliance. Due to its length, the 2015 edition of this comprehensive White Paper has been divided into three parts. Part 3 discusses the recommendations for large molecule bioanalysis using LBA, biomarkers and immunogenicity. Part 1 (small molecule bioanalysis using LCMS) and Part 2 (hybrid LBA/LCMS and regulatory inputs from major global health authorities) have been published in volume 7, issues 22 and 23 of Bioanalysis, respectively.

Published

2015

25. Recommendations for the development and validation of confirmatory anti-drug antibody assays

Author

Michele Fiscella, Thomas Klem, Lin Yang, Robin Marsden, Corinna Fiorotti, Heather Myler, Alvydas Mikulskis, Darshana Jani, and Carol Gleason

Subjects

Computer science, business.industry, Management science, Clinical Biochemistry, Antibodies, Monoclonal, General Medicine, Tiered approach, Anti-Drug Antibody, Analytical Chemistry, Biotechnology, Medical Laboratory Technology, Biopharmaceutical, Drug development, Drug Design, Antibody Formation, Humans, Biological Assay, General Pharmacology, Toxicology and Pharmaceutics, business, Antibody formation

Abstract

Identification and characterization of anti-drug antibodies is a critical component of biopharmaceutical drug development. The tiered approach for immunogenicity testing consists of screening, confirmatory, and characterization assays. Herein, we provide recommendations for confirmatory assays by expanding upon published guidance and present common practices across the industry. The authors recommend scientific approaches for development and validation of confirmatory assays using competition methods in ligand-binding assays, along with statistical formulae for routine use and validation. The paper will assist in understanding the confirmatory assay, and carefully implementing validation criteria a priori, as well as during sample analysis. These approaches represent the authors’ current knowledge and practices, with the aim that more uniform practices will be applied across the industry.

Published

2015

26. Biotransformation and stability of antibody-drug conjugates: payload metabolism and linker cleavage delineation

Author

Vangipuram S. Rangan, Alexander T. Kozhich, Shrikant Deshpande, Jian Wang, Renee Randazzo, and Heather Myler

Subjects

Drug, Immunoconjugates, Stereochemistry, media_common.quotation_subject, Clinical Biochemistry, Cleavage (embryo), Chemistry Techniques, Analytical, Analytical Chemistry, Biotransformation, Drug Stability, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, media_common, biology, Chemistry, Protein Stability, Payload (computing), General Medicine, Metabolism, Medical Laboratory Technology, Biochemistry, Pharmaceutical Preparations, biology.protein, Antibody, Linker, Conjugate

Published

2015

27. Anti-PEG antibody bioanalysis: a clinical case study with PEG-IFN-λ-1a and PEG-IFN-α2a in naive patients

Author

Heather Myler, Tonya Felix, George Kong, Murli Krishna, Carol Gleason, E. Cooney, Steven P. Piccoli, Robert Dodge, Binodh DeSilva, Subasree Srinivasan, Matthew Hruska, and Jie Zhu

Subjects

Bioanalysis, Clinical Biochemistry, Molecular Conformation, Immunoglobulins, macromolecular substances, Polyethylene glycol, Cross Reactions, Analytical Chemistry, Polyethylene Glycols, Therapy naive, chemistry.chemical_compound, PEG ratio, Medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Immunoassay, biology, business.industry, technology, industry, and agriculture, Cross reactions, Interferon-alpha, Reproducibility of Results, General Medicine, Hepatitis C, Medical Laboratory Technology, Titer, chemistry, Immunoglobulin M, Immunology, biology.protein, Clinical case, Antibody, business

Abstract

Background: Extensive use of polyethylene glycol (PEG) in consumer products necessitates the assessment of anti-PEG antibodies (APAb). Methods: In clinical trials comparing PEG-IFN-λ to PEG-IFN-α, conventional bridge and direct assays were assessed. Results & Conclusion: The bridge assay detected IgM and IgG APAb reactive with common PEG sizes and derivatives at sufficient sensitivity, 15–500 ng/ml. Of subjects evaluated, 6% of PEG-IFN-λ and 9% of PEG-IFN-α subjects had persistent APAb while 60% of PEG-IFN-λ and 33% of PEG-IFN-α subjects had persistent anti-interferon antibodies (AIAb). Pre-existing APAb and AIAb prevalence was comparable (approximately 10% of subjects). APAb were earlier onset, less frequent, less persistent and lower titer than AIAb. No associated hypersensitivity events were reported.

Published

2015

28. The pharmacokinetics of peginterferon lambda-1a following single dose administration to subjects with impaired renal function

Author

Matthew W, Hruska, Robert, Adamczyk, Elizabeth, Colston, Michael, Hesney, Michele, Stonier, Heather, Myler, and Richard, Bertz

Subjects

Adult, Adolescent, Interleukins, Middle Aged, Antiviral Agents, Severity of Illness Index, Polyethylene Glycols, Young Adult, Area Under Curve, Linear Models, Humans, Kidney Failure, Chronic, Pharmacokinetics, Aged, Glomerular Filtration Rate

Abstract

This open label study was conducted to assess the effect of renal impairment (RI) on the pharmacokinetics (PK) of peginterferon lambda-1a (Lambda).Subjects (age 18-75 years, BMI 18-35 kg m(-2) ) were enrolled into one of five renal function groups: normal (n = 12), mild RI (n = 8), moderate RI (n = 8), severe RI (n = 7), end-stage renal disease (ESRD, n = 8) based on estimated glomerular filtration rate (eGFR) calculated using the Modification of Diet in Renal Disease (MDRD) equation. Subjects received a single dose of Lambda (180 µg) subcutaneously on day 1 followed by PK serum sample collections through day 29. Safety, tolerability and immunogenicity data were collected through day 43. PK parameters were estimated and summarized by group. Geometric mean ratios (GMR) and 90% confidence intervals (CIs) were calculated between normal and RI groups.With decreasing eGFR, Lambda exposure (Cmax , AUC) increased while apparent clearance (CL/F) and apparent volume of distribution (V/F) decreased. Relative to subjects with normal renal function (geometric mean AUC = 99.5 ng ml(-1) h), Lambda exposure estimates (AUC) were slightly increased in the mild RI group (geometric mean [90% CI]: 1.20 [0.82, 1.77]) and greater in the moderate (1.95 [1.35, 2.83]), severe RI (1.95 [1.30, 2.93]) and ESRD (1.88 [1.30, 2.73]) groups. Lambda was generally well tolerated.The results demonstrated that RI reduces the clearance of Lambda and suggests that dose modifications may not be required in patients with mild RI but may be required in patients with moderate to severe RI or ESRD.

Published

2014

29. New FDA Draft Guidance on Immunogenicity

Author

Amy S. Rosenberg, Lakshmi Amaravadi, Valerie Quarmby, Ashwin Parenky, Karoline Bechtold-Peters, Heather Myler, and Susan Kirshner

Subjects

business.industry, Immunogenicity, media_common.quotation_subject, Pharmaceutical Science, Pharmacy, Meeting Report, Biotechnology, Food and drug administration, Patient safety, Presentation, Biopharmaceutical, Medicine, Engineering ethics, Session (computer science), business, Risk management, health care economics and organizations, media_common

Abstract

A “Late Breaking” session was held on May 20 at the 2013 American Association of Pharmaceutical Scientists-National Biotech Conference (AAPS-NBC) to discuss the US Food and Drug Administration’s (FDA) 2013 draft guidance on Immunogenicity Assessment for Therapeutic Protein Products. The session was initiated by a presentation from the FDA which highlighted several key aspects of the 2013 draft guidance pertaining to immunogenicity risk, the potential impact on patient safety and product efficacy, and risk mitigation. This was followed by an open discussion on the draft guidance which enabled delegates from biopharmaceutical companies to engage the FDA on topics that had emerged from their review of the draft guidance. The multidisciplinary audience fostered an environment that was conducive to scientific discussion on a broad range of topics such as clinical impact, immune mitigation strategies, immune prediction and the role of formulation, excipients, aggregates, and degradation products in immunogenicity. This meeting report highlights several key aspects of the 2013 draft guidance together with related dialog from the session.

Published

2014

30. A Protein Containing a Serine-rich Domain with Vesicle Fusing Properties Mediates Cell Cycle-dependent Cytosolic pH Regulation

Author

Derrick T. Brazill, Debra A. Brock, Robin R. Ammann, R. Diane Hatton, David R. Caprette, Heather Myler, Richard H. Gomer, and David F. Lindsey

Subjects

Vesicle fusion, Endocytic cycle, Protozoan Proteins, Cell Cycle Proteins, Biology, Membrane Fusion, Biochemistry, Catalysis, Cytosol, Serine, Asymmetric cell division, Animals, Dictyostelium, Molecular Biology, DNA Primers, Organelles, Base Sequence, Vesicle, Cell Cycle, Lipid bilayer fusion, Cell Biology, Hydrogen-Ion Concentration, Cell cycle, Cell biology, Microscopy, Electron, Endocytic vesicle

Abstract

Initial differentiation in Dictyostelium involves both asymmetric cell division and a cell cycle-dependent mechanism. We previously identified a gene, rtoA, which when disrupted randomizes the cell cycle-dependent mechanism without affecting either the underlying cell cycle or asymmetric differentiation. We find that in wild-type cells, RtoA levels vary during the cell cycle. Cytosolic pH, which normally varies with the cell cycle, is randomized in rtoA cells. The middle 60% of the RtoA protein is 10 tandem repeats of an 11 peptide-long serine-rich motif, which we find has a random coil structure. This domain catalyzes the fusion of phospholipid vesicles in vitro. Conversely, rtoA cells have a defect in the fusion of endocytic vesicles. They also have a decreased exocytosis rate, a decreased pH of endocytic/exocytic vesicles, and an increased average cytosolic pH. Our data indicate that the serine-rich domain of RtoA can mediate membrane fusion and that RtoA can increase the rate of vesicle fusion during processing of endoctyic vesicles. We hypothesize that RtoA modulates initial cell type choice by linking vegetative cell physiology to the cell cycle.

Published

2000

31. Large molecule specific assay operation: recommendation for best practices and harmonization from the global bioanalysis consortium harmonization team

Author

Heather Myler, Lauren Stevenson, Boris Gorovits, Karolina Österlund, Mario Dominguez, Yoshiyuki Minamide, Clare Kingsley, Marian Kelley, and Arumugam Muruganandam

Subjects

Analyte, Bioanalysis, Risk analysis (engineering), Computer science, Best practice, Practice Guidelines as Topic, Pharmaceutical Science, Proteins, White Paper, Harmonization, Validation Studies as Topic, Simulation, Chemistry Techniques, Analytical

Abstract

The L2 Global Harmonization Team on large molecule specific assay operation for protein bioanalysis in support of pharmacokinetics focused on the following topics: setting up a balanced validation design, specificity testing, selectivity testing, dilutional linearity, hook effect, parallelism, and testing of robustness and ruggedness. The team additionally considered the impact of lipemia, hemolysis, and the presence of endogenous analyte on selectivity assessments as well as the occurrence of hook effect in study samples when no hook effect had been observed during pre-study validation.

Published

2013

32. Validation and life-cycle management of a quantitative ligand-binding assay for the measurement of Nulojix(®), a CTLA-4-Fc fusion protein, in renal and liver transplant patients

Author

Richard Tacey, Kelli R. Phillips, Laura Hay, Heather Myler, Valarie Coats, Edward Tabler, Mehmooda Shaikh, Bruce Stouffer, and Huijin Dong

Subjects

Adult, Male, Immunoconjugates, medicine.drug_class, medicine.medical_treatment, Recombinant Fusion Proteins, Clinical Biochemistry, Enzyme-Linked Immunosorbent Assay, Urine, Liver transplantation, Pharmacology, Monoclonal antibody, Sensitivity and Specificity, Analytical Chemistry, Abatacept, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Kidney transplantation, Monitoring, Physiologic, biology, business.industry, Ligand binding assay, Antibodies, Monoclonal, Reproducibility of Results, General Medicine, medicine.disease, Fusion protein, Kidney Transplantation, Liver Transplantation, Medical Laboratory Technology, Immunology, biology.protein, Regression Analysis, Female, Antibody, business, Immunosuppressive Agents, medicine.drug

Abstract

Background: Nulojix® is a fusion protein composed of the Fc portion of a human IgG1 linked to the extracellular modified domain of CTLA-4. Nulojix differs from another Bristol Myers Squibb product, Orencia® by two amino acids and was approved by the FDA on 15 June 2011 for the prophylaxis of organ rejection in adult patients receiving kidney transplant. Results: A sandwich ELISA utilizing two monoclonal antibodies against CTLA-4 was employed for Nulojix quantification and pharmacokinetic analysis. At least 17 analysts have qualified on the assay and contributed to reportable results over the last 7 years. In-study accuracy and precision demonstrate suitable performance: %bias within -4 to 4%, %CV ≤13% and total error within 6–15%. Incurred sample reanalysis was completed in applicable disease-state populations. The assay was automated and validated in additional clinical matrices (ascites and urine) and Nulojix quantification was validated in the presence of clinically relevant co-administered compounds. In 2011, the biotinylation procedure was modified meriting a regression change (quadratic to 4-parameter logistic) and associated partial validation. Conclusion: This long-term pharmacokinetic program provides a good example of the dynamic clinical environment and adaptation requirements of ligand-binding assays.

Published

2012

33. Biotherapeutic bioanalysis: a multi-indication case study review

Author

George Hristopoulos, Allison Given, Johanna R Mora, Karen Kolz, and Heather Myler

Subjects

medicine.medical_specialty, Bioanalysis, medicine.drug_class, Clinical Biochemistry, Disease, Computational biology, Pharmacology, Monoclonal antibody, Chemistry Techniques, Analytical, Analytical Chemistry, Internal medicine, medicine, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, Biological Products, Hematology, business.industry, Antibodies, Monoclonal, General Medicine, Fusion protein, Therapeutic modalities, Recombinant Proteins, Medical Laboratory Technology, Pharmaceutical Preparations, Infectious disease (medical specialty), business

Abstract

A thorough understanding of the structure and biology of a biotherapeutic is crucial to defining a suitable strategy for pharmacokinetic characterization in proof-of-concept disease models, toxicology species as well as the healthy and disease indication patient populations. This manuscript summarizes parameters that impact bioanalytical strategy for over 50 biotherapeutics indicated for the treatment of oncology, rheumatoid arthritis, allergy, multiple sclerosis, hematology, metabolism and infectious disease. We have addressed numerous therapeutic modalities including chimeric, humanized and fully human monoclonal antibodies, replacement proteins, peptides and fusion proteins, including polyethylene glycol and Fc fusions, as well as antibody–drug conjugates. With the rapid evolution of biotherapeutics over the last 20 years and the contraction of the pharmaceutical and biotechnology labor force, efficient workflow management becomes a crucial bioanalytical component. Thus, we have also addressed new technologies that have demonstrated either increased throughput or enhanced characterization, including Meso Scale Discovery, Gyrolab and affinity MS.

Published

2011

34. Bioanalytical Approaches to Quantify 'Total' and 'Free' Therapeutic Antibodies and Their Targets: Technical Challenges and PK/PD Applications Over the Course of Drug Development

Author

Ago B. Ahene, Jihong Yang, Hossein Salimi-Moosavi, Meina T. Tang, Jian-Feng Lu, John Kamerud, Heather Myler, Lindsay King, Jean W. Lee, Marian Kelley, and Cindy Rogers

Subjects

Bioanalysis, Chemistry, medicine.drug_class, Ligand binding assay, Receptors, Drug, Pharmaceutical Science, White Paper, Antibodies, Monoclonal, Computational biology, Pharmacology, Monoclonal antibody, Ligands, Pharmacokinetics, Drug development, In vivo, Pharmacodynamics, Drug Design, medicine, Animals, Humans, PK/PD models, Algorithms

Abstract

The predominant driver of bioanalysis in supporting drug development is the intended use of the data. Ligand-binding assays (LBA) are widely used for the analysis of protein biotherapeutics and target ligands (L) to support pharmacokinetics/pharmacodynamics (PK/PD) and safety assessments. For monoclonal antibody drugs (mAb), in particular, which non-covalently bind to L, multiple forms of mAb and L can exist in vivo, including free mAb, free L, and mono- and/or bivalent complexes of mAb and L. Given the complexity of the dynamic binding equilibrium occurring in the body after dosing and multiple sources of perturbation of the equilibrium during bioanalysis, it is clear that ex vivo quantification of the forms of interest (free, bound, or total mAb and L) may differ from the actual ones in vivo. LBA reagents and assay formats can be designed in principle to measure the total or free forms of mAb and L. However, confirmation of the forms being measured under the specified conditions can be technically challenging. The assay forms and issues must be clearly communicated and understood appropriately by all stakeholders as the program proceeds through the development process. This paper focuses on monoclonal antibody biotherapeutics and their circulatory L that are either secreted as soluble forms or shed from membrane receptors. It presents an investigation into the theoretical and practical considerations for total/free analyte assessment to increase awareness in the scientific community and offer bioanalytical approaches to provide appropriate PK/PD information required at specific phases of drug development.

Published

2011

35. Troubleshooting PEG-hGH detection supporting pharmacokinetic evaluation in growth hormone deficient patients

Author

Juergen Kratzsch, Heather Myler, and Sami McVay

Subjects

Cross Reactions, Toxicology, Neutralization, Acid dissociation constant, Polyethylene Glycols, Drug detection, Matrix (chemical analysis), chemistry.chemical_compound, Mice, Pharmacokinetics, Growth hormone-binding protein, Antibody Specificity, Animals, Humans, Immunosorbent Techniques, Pharmacology, HEPES, Chromatography, Chemistry, Human Growth Hormone, Reproducibility of Results, Reference Standards, Biochemistry, Immunoglobulin M, Delayed-Action Preparations, Growth Hormone, Immunoglobulin G, PEGylation, Indicators and Reagents, Acids

Abstract

Introduction The ability to quantify systemic concentrations of protein therapeutics is complicated by the presence of endogenous analyte, specific binding proteins, and nonspecific matrix components in biological matrices ( Lee & Ma, 2007 ). Further complications can be introduced following pegylation whereby polyethylene glycol (PEG) impedes epitope recognition. Due to substantial interference from high affinity binding proteins and the inability to measure systemic drug concentrations under normal conditions, acid dissociation was implemented to facilitate the pharmacokinetic evaluation of clinical samples containing pegylated human growth hormone (PEG-hGH). Methods A sandwich electrochemiluminescent immunosorbent assay (ECLA) was employed using an anti-PEG capture, anti-hGH detection format, thereby eliminating cross-reactivity with endogenous compound. Samples were acid treated with glycine buffered hydrochloric acid (∼ pH 2.0) to dissociate PEG-hGH from serum resident growth hormone binding protein (GHBP; 3). After neutralization with a HEPES-based neutralizing buffer, samples were diluted in a casein-based assay buffer containing 0.2% I-block, 0.1% Tween-20, 2 M NaCl, and 10% normal mouse serum to eliminate nonspecific matrix effects. Meso Scale Discovery (MSD™) technology was employed to achieve sensitivity requirements. Results The drug detection assay was validated in the presence and absence of acid dissociation. Validation parameters included: intra- and inter-assay accuracy and precision, selectivity (> 60 lots of normal and growth hormone deficient human serum), cross-reactivity/specificity (Genotropin, hemoglobin, lipid, and bilirubin), dilutional linearity and stability (DeSilva et al., 2003; Shah et al., 1992; Smolec et al., 2005 Viswanathan et al., 2007; Food and Drug Administration, 2001). A 10-fold molar excess of GHBP was found to decrease PEG-hGH detection by > 90% while acid dissociation was shown to recover > 80% of the analyte. PEG-hGH clinical pharmacokinetic samples were analyzed with and without acid treatment. Only 38% of the mid-dose samples were quantifiable without acid treatment while 92% were quantifiable after acid dissociation. Discussion The implementation of acid dissociation was found to substantially increase the number of quantifiable pharmacokinetic samples over the drug exposure time course and contributed significantly to the robustness of pharmacokinetic evaluation.

Published

2009

36. Novel heparanase-inhibiting antibody reduces neointima formation

Author

Elizabeth A. Lipke, Heather Myler, Jennifer L. West, and Elizabeth Rice

Subjects

Neointima, Male, Cell, Basic fibroblast growth factor, Myocytes, Smooth Muscle, Biochemistry, Antibodies, Extracellular matrix, Rats, Sprague-Dawley, chemistry.chemical_compound, Restenosis, Platelet degranulation, medicine, Animals, Heparanase, Molecular Biology, Glucuronidase, biology, Chemistry, General Medicine, medicine.disease, Rats, medicine.anatomical_structure, Carotid Arteries, Immunology, cardiovascular system, biology.protein, Cancer research, Fibroblast Growth Factor 2, Antibody

Abstract

Basic fibroblast growth factor (bFGF), stored bound to heparan sulfate proteoglycans in the extracellular matrix (ECM) of the arterial media, may initiate smooth muscle cell (SMC) proliferation after coronary intervention, thus contributing to restenosis. bFGF mobilization from ECM stores after injury may be induced by platelet degranulation products such as heparanase. Therapies aimed at the inhibition of bFGF release and activation may assist in prevention of restenosis. To test this theory, we first examined the mobilization and activation of bFGF in the arterial media by platelet-derived heparanase. Heparanase, locally delivered to the rat carotid artery, was found to release bFGF and induce substantial SMC proliferation in the absence of actual vascular injury. An antibody that neutralizes heparanase was then developed and evaluated in a rat carotid balloon injury model. Local delivery of anti-heparanase IgG was found to inhibit bFGF release by approximately 60% ( p < 0.001) at 4 d; this correlated with the significant reduction in neointima formation observed at 14 d (intimal area/medial area: control 1.3 +/- 0.3, anti-heparanase 0.35 +/- 0.12, p < 0.0001). Platelet-derived heparanase is therefore likely to be important in initiating events leading to restenosis via bFGF mobilization. Furthermore, heparanase neutralization may assist in the prevention of restenosis following vascular injury.

Published

2006

37. Nitric oxide-generating hydrogels inhibit neointima formation

Author

Corinna C. Zygourakis, Heather Myler, Elizabeth A. Lipke, David A. Tulis, Elizabeth Rice, Kristyn S. Bohl Masters, Jennifer L. West, and Meghan S. Liel

Subjects

Neointima, Male, Materials science, Myocytes, Smooth Muscle, Biomedical Engineering, Biophysics, Bioengineering, Nitric Oxide, Nitric oxide, Biomaterials, Rats, Sprague-Dawley, chemistry.chemical_compound, Platelet Adhesiveness, Cell Movement, PEG ratio, Cell Adhesion, Animals, Nitric Oxide Donors, Cysteine, Angioplasty, Balloon, Coronary, Cyclic GMP, Cells, Cultured, Cell Proliferation, S-Nitrosothiols, Cell growth, Endothelial Cells, Hydrogels, Anatomy, Extracellular Matrix, Rats, Endothelial stem cell, Carotid Arteries, chemistry, Covalent bond, Drug delivery, Self-healing hydrogels, Tunica Intima

Abstract

This study evaluated the effects of localized delivery of nitric oxide (NO) from hydrogels covalently modified with S-nitrosocysteine (Cys-NO) on neoinitma formation, a key component of restenosis, in a rat balloon-injury model. Soluble Cys-NO was used in preliminary studies to identify dosage ranges that were able to simultaneously inhibit smooth muscle cell proliferation, enhance endothelial cell proliferation, and reduce platelet adhesion. Photo-cross-linked PEG-based hydrogels were formed with covalently immobilized Cys-NO. These materials release NO for approximately 24 h and can be applied to tissues and photo-cross-linked in situ to form local drug-delivery systems. Localized delivery of NO from hydrogels containing Cys-NO inhibited neointima formation in a rat balloon-injury model by approximately 75% at 14 days.

Published

2005

38. Nitric-oxide generating hydrogels inhibit intimal thickening and promote endothelial cell proliferation

Author

Heather Myler, Elizabeth A. Lipke, C. Shen, Kristyn S. Bohl Masters, and Jennifer L. West

Subjects

Cell growth, medicine.medical_treatment, Adhesion, Pharmacology, medicine.disease, Nitric oxide, Endothelial stem cell, chemistry.chemical_compound, Restenosis, chemistry, Angioplasty, Self-healing hydrogels, medicine, Cell adhesion, Biomedical engineering

Abstract

Nitric oxide-generating hydrogels have been shown to inhibit smooth muscle cell proliferation and platelet adhesion, as well as promote endothelial cell proliferation; for this reason these hydrogels should be useful in preventing restenosis, or vessel re-occlusion, following balloon angioplasty. Over 600,000 percutaneous transluminal coronary angioplasty (PTCA) procedures are performed annually in the U.S.; unfortunately. 30-40% of patients treated with PTCA experience failure due to restenosis. We have developed nitric oxide (NO)-generating hydrogels that release NO over a period of days to weeks, depending on material design. They are able to significantly reduce platelet adhesion to collagen and inhibit smooth muscle cell proliferation in vitro. In addition, we have covalently grafted a cell adhesion peptide into the NO-generating hdrogels and assessed the ability of endothelial cells (EC) to proliferate on the surface. ECs owed significantly higher rates of proliferation on the NO-generating hydrogels as compared to controls. The perivascular application of NO-generating, hydrogels significantly reduced neointimal formation in an experimental balloon angioplasty model as compared to controls. The combined effects of these NO-generating hydrogels make them well suited for incorporation into blood-contacting devices and for use as a stent coating or stent replacement to prevent restenosis following balloon angioplasty.

Published

2003

39. Heparanase and platelet factor-4 induce smooth muscle cell proliferation and migration via bFGF release from the ECM

Author

Jennifer L. West and Heather Myler

Subjects

Blood Platelets, medicine.medical_treatment, Basic fibroblast growth factor, Platelet Factor 4, Biochemistry, Extracellular matrix, chemistry.chemical_compound, Plasminogen Activators, Platelet degranulation, Cell Movement, medicine, Humans, Heparanase, Platelet activation, Molecular Biology, Cells, Cultured, Glucuronidase, Growth factor, Cell migration, Muscle, Smooth, General Medicine, Cell biology, Extracellular Matrix, chemistry, Immunoglobulin G, cardiovascular system, Fibroblast Growth Factor 2, Platelet factor 4, Cell Division

Abstract

Basic fibroblast growth factor (bFGF) has been shown to play an instrumental role in the cascade of events leading to restenosis; however, the mechanisms of bFGF activation following vascular injury have remained elusive. We have demonstrated that heparanase and platelet factor-4 (PF4), released from activated platelets at the site of injury, liberate bFGF from the extracellular matrix (ECM) of vascular smooth muscle cells (SMC), resulting in the induction of SMC proliferation and migration. Increases in proliferation and migration were inhibited by treatment with a bFGF-neutralizing antibody, suggesting that proliferation and migration in response to heparanase or PF4 are mediated by bFGF activation. When platelets were seeded on top of SMCs, degranulation products were found to release bFGF from the ECM, increasing cell proliferation and cell migration. Again, these increases in SMC proliferation and migration were inhibited by treatment with an anti-bFGF antibody. Furthermore, these increases in proliferation were completely inhibited by treatment with an anti-heparanase antibody. Platelet degranulation products, such as heparanase and PF4, may liberate bFGF from extracellular sequestration, activating the growth factor and inducing the SMC proliferation and migration that contribute to the wound healing response following vascular injury.

Published

2002