| Literature DB >> 28380339 |
Haiyan Hong1, Yongfei Cai1, Shijun Zhang1, Hongyan Ding1, Haitao Wang2, Aidong Han3.
Abstract
The NatB N-terminal acetyltransferase specifically acetylates the N-terminal group of substrate protein peptides starting with Met-Asp/Glu/Asn/Gln. How NatB recognizes and acetylates these substrates remains unknown. Here, we report crystal structures of a NatB holoenzyme from Candida albicans in the presence of its co-factor CoA and substrate peptides. The auxiliary subunit Naa25 of NatB forms a horseshoe-like deck to hold specifically its catalytic subunit Naa20. The first two amino acids Met and Asp of a substrate peptide mediate the major interactions with the active site in the Naa20 subunit. The hydrogen bonds between the substrate Asp and pocket residues of Naa20 are essential to determine the NatB substrate specificity. Moreover, a hydrogen bond between the amino group of the substrate Met and a carbonyl group in the Naa20 active site directly anchors the substrate toward acetyl-CoA. Together, these structures define a unique molecular mechanism of specific N-terminal acetylation acted by NatB.Entities:
Keywords: N-terminal acetylation; N-terminal acetyltransferase; NatB; acetylation; crystal structure; protein post-translational modification
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Year: 2017 PMID: 28380339 DOI: 10.1016/j.str.2017.03.003
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006