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Both positional and chemical variables control in vitro proteolytic cleavage of a presenilin ortholog

J Biol Chem.. 2018-03; 
Naing SH, Kalyoncu S, Smalley DM, Kim H, Tao X, George JB, Jonke AP, Oliver RC, Urban VS, Torres MP, Lieberman RL.
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摘要

Mechanistic details of intramembrane aspartyl protease (IAP) chemistry, which is central to many biological and pathogenic processes, remain largely obscure. Here, we investigated the in vitro kinetics of a microbial intramembrane aspartyl protease (mIAP) fortuitously acting on the renin substrate angiotensinogen and the C-terminal transmembrane segment of amyloid precursor protein (C100), which is cleaved by the presenilin subunit of γ-secretase, an Alzheimer disease (AD)-associated IAP. mIAP variants with substitutions in active-site and putative substrate-gating residues generally exhibit impaired, but not abolished, activity toward angiotensinogen and retain the predominant cleavage site (His-Thr). The aro... More

关键词

Alzheimer disease; amyloid precursor protein (APP); enzyme kinetics; intramembrane proteolysis; mass spectrometry (MS); membrane enzyme; neurodegenerative disease; presenilin; substrate specificity