SARM1 orthosteric base exchange inhibitors cause subinhibitory SARM1 activation

Rebecca Leahey
Martin Weber
Chang Hoon Cho
Seong Hur
Amber Cramer
Karla Manzanares
Brett Babin
Gladys Boenig
Taylor Kring
Liling Liu
Yusi Cui
Anjani Ganti
John P. Evans
Marika Nespi
Justin Ly
Alicia A. Nugent
Samantha Green
Bryan Chan
Casper C. Hoogenraad
Anton Delwig
Flora I. Hinz

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Abstract

SARM1, an octameric NADase, is a key regulator of axon degeneration and an emerging target in small molecule drug discovery to treat a wide range of neurodegenerative diseases. Recently, a structurally diverse series of adduct-forming, orthosteric SARM1 inhibitors have been discovered. Here, we show that subinhibitory concentrations of these orthosteric inhibitors, under mildly SARM1 activating conditions, cause sustained SARM1 activation. This synergistic adverse effect leads to increased nicotinamide adenine dinucleotide (NAD) consumption, neurodegeneration and release of the biomarker neurofilament-light (NfL) in cultured cortical neurons. In two distinct animal models, we found that low-dose treatment with these orthosteric SARM1 inhibitors results in increased plasma NfL and adverse events when combined with cellular stress or injury conditions. This may present a critical liability for orthosteric SARM1 inhibitors in certain patient populations.

Version published to 10.1101/2024.08.06.606489v1 on bioRxiv
Aug 8, 2024

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