Literature DB >> 29271699

Establishing in vitro in vivo correlations to screen monoclonal antibodies for physicochemical properties related to favorable human pharmacokinetics.

Lindsay B Avery1, Jason Wade2, Mengmeng Wang1, Amy Tam2, Amy King2, Nicole Piche-Nicholas2, Mania S Kavosi1, Steve Penn1,3, David Cirelli4, Jeffrey C Kurz1, Minlei Zhang1, Orla Cunningham5, Rhys Jones2,6, Brian J Fennell5, Barry McDonnell5, Paul Sakorafas4, James Apgar2, William J Finlay5,7, Laura Lin2, Laird Bloom2, Denise M O'Hara1.   

Abstract

Implementation of in vitro assays that correlate with in vivo human pharmacokinetics (PK) would provide desirable preclinical tools for the early selection of therapeutic monoclonal antibody (mAb) candidates with minimal non-target-related PK risk. Use of these tools minimizes the likelihood that mAbs with unfavorable PK would be advanced into costly preclinical and clinical development. In total, 42 mAbs varying in isotype and soluble versus membrane targets were tested in in vitro and in vivo studies. MAb physicochemical properties were assessed by measuring non-specific interactions (DNA- and insulin-binding ELISA), self-association (affinity-capture self-interaction nanoparticle spectroscopy) and binding to matrix-immobilized human FcRn (surface plasmon resonance and column chromatography). The range of scores obtained from each in vitro assay trended well with in vivo clearance (CL) using both human FcRn transgenic (Tg32) mouse allometrically projected human CL and observed human CL, where mAbs with high in vitro scores resulted in rapid CL in vivo. Establishing a threshold value for mAb CL in human of 0.32 mL/hr/kg enabled refinement of thresholds for each in vitro assay parameter, and using a combinatorial triage approach enabled the successful differentiation of mAbs at high risk for rapid CL (unfavorable PK) from those with low risk (favorable PK), which allowed mAbs requiring further characterization to be identified. Correlating in vitro parameters with in vivo human CL resulted in a set of in vitro tools for use in early testing that would enable selection of mAbs with the greatest likelihood of success in the clinic, allowing costly late-stage failures related to an inadequate exposure profile, toxicity or lack of efficacy to be avoided.

Entities:  

Keywords:  AC-SINS; FcRn binding; IgG; clearance, in vitro assays; mAb; monoclonal antibody, neonatal Fc receptor; pharmacokinetics; polyreactivity

Mesh:

Substances:

Year:  2018        PMID: 29271699      PMCID: PMC5825195          DOI: 10.1080/19420862.2017.1417718

Source DB:  PubMed          Journal:  MAbs        ISSN: 1942-0862            Impact factor:   5.857


  48 in total

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Authors:  Miroslav Dostalek; Thomayant Prueksaritanont; Robert F Kelley
Journal:  MAbs       Date:  2017-05-02       Impact factor: 5.857

2.  Rapid analysis of antibody self-association in complex mixtures using immunogold conjugates.

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3.  One mouse, one pharmacokinetic profile: quantitative whole blood serial sampling for biotherapeutics.

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4.  Prediction of human pharmacokinetics of therapeutic monoclonal antibodies from simple allometry of monkey data.

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Journal:  Drug Metab Pharmacokinet       Date:  2011-05-24       Impact factor: 3.614

5.  Enhanced antibody half-life improves in vivo activity.

Authors:  Jonathan Zalevsky; Aaron K Chamberlain; Holly M Horton; Sher Karki; Irene W L Leung; Thomas J Sproule; Greg A Lazar; Derry C Roopenian; John R Desjarlais
Journal:  Nat Biotechnol       Date:  2010-01-17       Impact factor: 54.908

6.  Evidence to support the cellular mechanism involved in serum IgG homeostasis in humans.

Authors:  E Sally Ward; Jinchun Zhou; Victor Ghetie; Raimund J Ober
Journal:  Int Immunol       Date:  2003-02       Impact factor: 4.823

7.  Evaluating the Use of Antibody Variable Region (Fv) Charge as a Risk Assessment Tool for Predicting Typical Cynomolgus Monkey Pharmacokinetics.

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Journal:  J Biol Chem       Date:  2015-10-21       Impact factor: 5.157

Review 8.  Interspecies scaling of therapeutic monoclonal antibodies: initial look.

Authors:  Jie Ling; Honghui Zhou; Qun Jiao; Hugh M Davis
Journal:  J Clin Pharmacol       Date:  2009-10-16       Impact factor: 3.126

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Journal:  Drugs       Date:  2009       Impact factor: 9.546

10.  Charge-mediated influence of the antibody variable domain on FcRn-dependent pharmacokinetics.

Authors:  Angela Schoch; Hubert Kettenberger; Olaf Mundigl; Gerhard Winter; Julia Engert; Julia Heinrich; Thomas Emrich
Journal:  Proc Natl Acad Sci U S A       Date:  2015-04-27       Impact factor: 11.205

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Journal:  MAbs       Date:  2019-02-12       Impact factor: 5.857

2.  De novo discovery of antibody drugs - great promise demands scrutiny.

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3.  In vitro and in silico assessment of the developability of a designed monoclonal antibody library.

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Authors:  Charles G Starr; Peter M Tessier
Journal:  Curr Opin Biotechnol       Date:  2019-02-26       Impact factor: 9.740

Review 5.  Opportunities and Challenges for PBPK Model of mAbs in Paediatrics and Pregnancy.

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6.  High-throughput profiling of antibody self-association in multiple formulation conditions by PEG stabilized self-interaction nanoparticle spectroscopy.

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Journal:  MAbs       Date:  2022 Jan-Dec       Impact factor: 6.440

Review 7.  Current advances in biopharmaceutical informatics: guidelines, impact and challenges in the computational developability assessment of antibody therapeutics.

Authors:  Rahul Khetan; Robin Curtis; Charlotte M Deane; Johannes Thorling Hadsund; Uddipan Kar; Konrad Krawczyk; Daisuke Kuroda; Sarah A Robinson; Pietro Sormanni; Kouhei Tsumoto; Jim Warwicker; Andrew C R Martin
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8.  Assessment of Therapeutic Antibody Developability by Combinations of In Vitro and In Silico Methods.

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9.  Antibodies with Weakly Basic Isoelectric Points Minimize Trade-offs between Formulation and Physiological Colloidal Properties.

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10.  Identifying biophysical assays and in silico properties that enrich for slow clearance in clinical-stage therapeutic antibodies.

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Journal:  MAbs       Date:  2021 Jan-Dec       Impact factor: 5.857

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