Orthogonal analysis of dystrophin protein and mRNA as a surrogate outcome for drug development

Author:

Uaesoontrachoon Kitipong1,Srinivassane Sadish1,Warford Jordan1,Mekhssian Kevork2,Montpetit Hélène2,Beauvois Romain2,Keyhani Anahita2,Hathout Yetrib3,Yamashita Taishi4,Satou Youhei4,Osaki Hironori4,Praest Molly1,Moraca Marina1,Malbasic Maja1,Ross William1,MacKinnon Alexandra1,Rowsell Joyce1,Mullen Amanda1,Matyas Mark1,Mummidivarpu Swati3,Nagaraju Kanneboyina13,Hoffman Eric P13

Affiliation:

1. AGADA BioSciences Inc., Halifax, Nova Scotia B3H0A8, Canada

2. Altasciences, Laval, Québec H7V4B3, Canada

3. Binghamton University, SUNY. Binghamton, NY 13902, USA

4. NS Pharma, Inc., Paramus, NJ 07652, USA

Abstract

Aim: Detection of drug-induced dystrophin in patient muscle biopsy is a surrogate outcome measure for Duchenne muscular dystrophy. We sought to establish and validate an orthogonal approach to measurement of dystrophin protein and RNA in muscle biopsies. Materials & methods: Validated methods were developed for dystrophin western blotting, mass spectrometry, immunostaining and reverse transcriptase PCR of biopsy mRNA using muscle biopsy standards. Results: Both western blotting and mass spectrometry validated methods demonstrated good linearity, and acceptable precision and accuracy with a lower limit of quantitation at 1%. Immunostaining and reverse transcriptase PCR methods were shown to be reliable. Conclusion: The described orthogonal approach is sufficient to support measures of dystrophin as a surrogate outcome in a clinical trial.

Publisher

Future Medicine Ltd

Subject

Biochemistry (medical),Clinical Biochemistry,Drug Discovery

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