Literature DB >> 25800415

Translational development of an ADAMTS-5 antibody for osteoarthritis disease modification.

J Larkin1, T A Lohr2, L Elefante3, J Shearin4, R Matico4, J-L Su4, Y Xue3, F Liu5, C Genell6, R E Miller7, P B Tran7, A-M Malfait7, C C Maier6, C J Matheny8.   

Abstract

OBJECTIVE/
METHOD: Aggrecanase activity, most notably ADAMTS-5, is implicated in pathogenic cartilage degradation. Selective monoclonal antibodies (mAbs) to both ADAMTS-5 and ADAMTS-4 were generated and in vitro, ex vivo and in vivo systems were utilized to assess target engagement, aggrecanase inhibition and modulation of disease-related endpoints with the intent of selecting a candidate for clinical development in osteoarthritis (OA).
RESULTS: Structural mapping predicts the most potent mAbs employ a unique mode of inhibition by cross-linking the catalytic and disintegrin domains. In a surgical mouse model of OA, both ADAMTS-5 and ADAMTS-4-specific mAbs penetrate cartilage following systemic administration, demonstrating access to the anticipated site of action. Structural disease modification and associated alleviation of pain-related behavior were observed with ADAMTS-5 mAb treatment. Treatment of human OA cartilage demonstrated a preferential role for ADAMTS-5 inhibition over ADAMTS-4, as measured by ARGS neoepitope release in explant cultures. ADAMTS-5 mAb activity was most evident in a subset of patient-derived tissues and suppression of ARGS neoepitope release was sustained for weeks after a single treatment in human explants and in cynomolgus monkeys, consistent with high affinity target engagement and slow ADAMTS-5 turnover.
CONCLUSION: This data supports a hypothesis set forth from knockout mouse studies that ADAMTS-5 is the major aggrecanase involved in cartilage degradation and provides a link between a biological pathway and pharmacology which translates to human tissues, non-human primate models and points to a target OA patient population. Therefore, a humanized ADAMTS-5-selective monoclonal antibody (GSK2394002) was progressed as a potential OA disease modifying therapeutic.
Copyright © 2015 The Authors. Published by Elsevier Ltd.. All rights reserved.

Entities:  

Keywords:  ADAMTS-4; ADAMTS-5; Cartilage; Disease-modifying osteoarthritis drugs (DMOADs); Monoclonal antibody; Osteoarthritis

Mesh:

Substances:

Year:  2015        PMID: 25800415      PMCID: PMC4516626          DOI: 10.1016/j.joca.2015.02.778

Source DB:  PubMed          Journal:  Osteoarthritis Cartilage        ISSN: 1063-4584            Impact factor:   6.576


  49 in total

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Authors:  F M Germaschewski; C J Matheny; J Larkin; F Liu; L R Thomas; J S Saunders; K Sully; C Whittall; Y Boyle; G Peters; N M Graham
Journal:  Osteoarthritis Cartilage       Date:  2014-02-28       Impact factor: 6.576

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Review 10.  Proteases involved in cartilage matrix degradation in osteoarthritis.

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7.  Therapeutic effects of an anti-ADAMTS-5 antibody on joint damage and mechanical allodynia in a murine model of osteoarthritis.

Authors:  R E Miller; P B Tran; S Ishihara; J Larkin; A M Malfait
Journal:  Osteoarthritis Cartilage       Date:  2015-09-26       Impact factor: 6.576

8.  A Disintegrin and Metalloproteinase with Thrombospondin Motifs-5 (ADAMTS-5) Forms Catalytically Active Oligomers.

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