期刊
ELIFE
卷 10, 期 -, 页码 -出版社
eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.67381
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资金
- Ministry of Science and Technology of the People's Republic of China [2019YFA0906000]
- National Science Foundation of China [31871401]
- Hong Kong Baptist University [RC-SGT2/18-19/SCI/005, RC-ICRS-18-19-01A]
By designing and synthesizing specific fluorescent conjugates, the activation process of SARM1 was predicted and visualized, while a derivative of nisoldipine was found to inhibit SARM1 activation, protecting neuronal axons from degeneration.
SARM1 regulates axonal degeneration through its NAD-metabolizing activity and is a drug target for neurodegenerative disorders. We designed and synthesized fluorescent conjugates of styryl derivative with pyridine to serve as substrates of SARM1, which exhibited large red shifts after conversion. With the conjugates, SARM1 activation was visualized in live cells following elevation of endogenous NMN or treatment with a cell-permeant NMN-analog. In neurons, imaging documented mouse SARM1 activation preceded vincristine-induced axonal degeneration by hours. Library screening identified a derivative of nisoldipine (NSDP) as a covalent inhibitor of SARM1 that reacted with the cysteines, especially Cys311 in its ARM domain and blocked its NMN-activation, protecting axons from degeneration. The Cryo-EM structure showed that SARM1 was locked into an inactive conformation by the inhibitor, uncovering a potential neuroprotective mechanism of dihydropyridines.
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