Issue 12, 2018

The transition to magic bullets – transition state analogue drug design

Abstract

In the absence of industry partnerships, most academic groups lack the infrastructure to rationally design and build drugs via methods used in industry. Instead, academia needs to work smarter using mechanism-based design. Working smarter can mean the development of new drug discovery paradigms and then demonstrating their utility and reproducibility to industry. The collaboration between Vern Schramm's group at the Albert Einstein College of Medicine, USA and Peter Tyler at the Ferrier Research Institute at The Victoria University of Wellington, NZ has refined a drug discovery process called transition state analogue design. This process has been applied to several biomedically relevant nucleoside processing enzymes. In 2017, Mundesine®, conceived using transition state analogue design, received market approval for the treatment of peripheral T-cell lymphoma in Japan. This short review looks at a brief history of transition state analogue design, the fundamentals behind the development of this process, and the success of enzyme inhibitors produced using this drug design methodology.

Graphical abstract: The transition to magic bullets – transition state analogue drug design

Article information

Article type
Review Article
Submitted
25 Jul 2018
Accepted
24 Aug 2018
First published
28 Aug 2018

Med. Chem. Commun., 2018,9, 1983-1993

The transition to magic bullets – transition state analogue drug design

G. B. Evans, V. L. Schramm and P. C. Tyler, Med. Chem. Commun., 2018, 9, 1983 DOI: 10.1039/C8MD00372F

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