The Rise and Fall of SARM1 Base-Exchange Inhibitors

Thomas Lundbäck
Vijay Chandrasekar
Chendi Gu
Hyoungseok Ju
Robyn McAdam
Maria Palomero
Kasim Sader
Bradley Peter
Lisa Wissler
Philip Nevin
Edmund Foster
Tanguy Jamier
Pravallika Manjappa
Carina Johansson
Jenny Sandmark
Mei Ding
Anette Persson-Kry
Sanhita Mitra
Tugce Munise Satir
Bilada Bilican
Mirko Messa
Graham Fraser
John Linley
Helen Plant
Rachel Moore
Tina Seifert
Michael Lerche
Carina Raynochek
Ewa Nilsson
Nour Majbour
Richard Lucey
Taiana Maia de Oliveira
Qi Wang
Iain Chessell
Perla Breccia
Rebecca Jarvis

0 evaluations Published on Nov 12, 2025

This article on Sciety

Abstract

The sterile alpha and TIR motif containing 1 (SARM1) enzyme is a key driver of axonal degeneration in response to injury, making it an attractive target for treating chemotherapy-induced peripheral neuropathy (CIPN) and other nervous system diseases. In this study, we identified and optimised a new class of base-exchange inhibitors (BEXi) targeting SARM1 and explored their molecular interactions and conformational effects using cryo-EM, HDX-MS and SAXS. Although BEXi produced robust inhibition across all biochemical and cellular assay formats, application at sub-inhibitory concentrations consistently led to paradoxical SARM1 activation, and in neuronal assays, accelerated neurite degeneration. Further analysis showed that BEXi only delayed, rather than prevented, neurite degeneration when applied to primary neuronal cells, even at exceedingly high inhibitor concentrations. These results prompted us to discontinue BEXi development in favour of alternative strategies, underscoring the complexity of SARM1 as a therapeutic target and the need for comprehensive, mechanistically informed screening cascades.

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