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Unique Structural Features of the Mitochondrial AAA+ Protease AFG3L2 Reveal the Molecular Basis for Activity in Health and Disease.

Mol Cell. 2019; 
Puchades Cristina,Ding Bojian,Song Albert,Wiseman R Luke,Lander Gabriel C,Glynn Stev
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Catalog Peptides Fluorogenic peptide cleavage assays were performed at 37C with 1 mM coreAFG3L2WB or its variants and 50 mM peptide (Leu-(3-NO2-Tyr)-Phe-Gly-(Lys-Abz)) (GenScript) (Key Resources Table) in a 384-well black plate using SpectraMax M5 plate reader (ex = 320 nm; em = 420 nm). Get A Quote

摘要

Mitochondrial AAA+ quality-control proteases regulate diverse aspects of mitochondrial biology through specialized protein degradation, but the underlying mechanisms of these enzymes remain poorly defined. The mitochondrial AAA+ protease AFG3L2 is of particular interest, as genetic mutations localized throughout AFG3L2 are linked to diverse neurodegenerative disorders. However, a lack of structural data has limited our understanding of how mutations impact enzymatic function. Here, we used cryoelectron microscopy (cryo-EM) to determine a substrate-bound structure of the catalytic core of human AFG3L2. This structure identifies multiple specialized structural features that integrate with conserved motifs... More

关键词

AAA+ protease,mitochondrial quality control,neurodegenerative disease,spinocerebellar ataxia typ