Fragment optimization and elaboration strategies - the discovery of two lead series of PRMT5/MTA inhibitors from five fragment hits

Christopher R. Smith; Svitlana Kulyk; Misbha Ud Din Ahmad; Valentina Arkhipova; James G. Christensen; Robin J. Gunn; Anthony Ivetac; John M. Ketcham; Jon Kuehler; J. David Lawson; Nicole C. Thomas; Xiaolun Wang; Matthew A. Marx

Journal ArticleOPEN ACCESS

Fragment optimization and elaboration strategies - the discovery of two lead series of PRMT5/MTA inhibitors from five fragment hits

RSC Medicinal Chemistry (2022) 13(12) 1549-1564

DOI: 10.1039/d2md00163b

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Abstract

Here we describe the early stages of a fragment-based lead discovery (FBLD) project for a recently elucidated synthetic lethal target, the PRMT5/MTA complex, for the treatment of MTAP-deleted cancers. Starting with five fragment/PRMT5/MTA X-ray co-crystal structures, we employed a two-phase fragment elaboration process encompassing optimization of fragment hits and subsequent fragment growth to increase potency, assess synthetic tractability, and enable structure-based drug design. Two lead series were identified, one of which led to the discovery of the clinical candidate MRTX1719.

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Smith, C. R., Kulyk, S., Ahmad, M. U. D., Arkhipova, V., Christensen, J. G., Gunn, R. J., … Marx, M. A. (2022). Fragment optimization and elaboration strategies - the discovery of two lead series of PRMT5/MTA inhibitors from five fragment hits. RSC Medicinal Chemistry, 13(12), 1549–1564. https://doi.org/10.1039/d2md00163b

Fragment optimization and elaboration strategies - the discovery of two lead series of PRMT5/MTA inhibitors from five fragment hits

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