| Literature DB >> 28096333 |
Tushar Jain1, Tingwan Sun2, Stéphanie Durand3, Amy Hall3, Nga Rewa Houston3,4, Juergen H Nett5, Beth Sharkey5, Beata Bobrowicz5, Isabelle Caffry2, Yao Yu2, Yuan Cao2, Heather Lynaugh2, Michael Brown2, Hemanta Baruah4, Laura T Gray4, Eric M Krauland4, Yingda Xu6, Maximiliano Vásquez7, K Dane Wittrup7,2,3,4,5.
Abstract
Antibodies are a highly successful class of biological drugs, with over 50 such molecules approved for therapeutic use and hundreds more currently in clinical development. Improvements in technology for the discovery and optimization of high-potency antibodies have greatly increased the chances for finding binding molecules with desired biological properties; however, achieving drug-like properties at the same time is an additional requirement that is receiving increased attention. In this work, we attempt to quantify the historical limits of acceptability for multiple biophysical metrics of "developability." Amino acid sequences from 137 antibodies in advanced clinical stages, including 48 approved for therapeutic use, were collected and used to construct isotype-matched IgG1 antibodies, which were then expressed in mammalian cells. The resulting material for each source antibody was evaluated in a dozen biophysical property assays. The distributions of the observed metrics are used to empirically define boundaries of drug-like behavior that can represent practical guidelines for future antibody drug candidates.Entities:
Keywords: biophysical properties; developability; manufacturability; monoclonal antibody; nonspecificity
Mesh:
Substances:
Year: 2017 PMID: 28096333 PMCID: PMC5293111 DOI: 10.1073/pnas.1616408114
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205