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Molecular basis for N-terminal alpha-synuclein acetylation by human NatB

Elife. 2020; 
Sunbin Deng, Buyan Pan, Leah Gottlieb, E James Petersson, Ronen Marmorstein
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Peptide Synthesis … “VFMK” peptide: NH2- VFMKGLSRWGRPVGRRRRP -COOH; GenScript). Reactions were performed in triplicate. To determine steady-state catalytic parameters of hNatB with respect to acetyl-CoA, 100 nM hNatB was mixed with a saturating concentration … Get A Quote

摘要

NatB is one of three major N-terminal acetyltransferase (NAT) complexes (NatA-NatC), which co-translationally acetylate the N-termini of eukaryotic proteins. Its substrates account for about 21% of the human proteome, including well known proteins such as actin, tropomyosin, CDK2, and α-synuclein (αSyn). Human NatB (hNatB) mediated N-terminal acetylation of αSyn has been demonstrated to play key roles in the pathogenesis of Parkinson's disease and as a potential therapeutic target for hepatocellular carcinoma. Here we report the cryo-EM structure of hNatB bound to a CoA-αSyn conjugate, together with structure-guided analysis of mutational effects on catalysis. This analysis reveals functionally important di... More

关键词

Cryo-EM, N-terminal acetylation, NatB, human, molecular biophysics, structural biology, α-synuclein