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含FIC结构域的人类蛋白HYPE的晶体结构及其功能意义

Crystal structure of the human, FIC-domain containing protein HYPE and implications for its functions.

作者信息

Bunney Tom D, Cole Ambrose R, Broncel Malgorzata, Esposito Diego, Tate Edward W, Katan Matilda

机构信息

Division of Biosciences, Institute of Structural and Molecular Biology, University College London, Gower Street, London WC1E 6BT, UK.

Institute of Structural and Molecular Biology, Birkbeck College, London WC1 7HX, UK.

出版信息

Structure. 2014 Dec 2;22(12):1831-1843. doi: 10.1016/j.str.2014.10.007.

Abstract

Protein AMPylation, the transfer of AMP from ATP to protein targets, has been recognized as a new mechanism of host-cell disruption by some bacterial effectors that typically contain a FIC-domain. Eukaryotic genomes also encode one FIC-domain protein,HYPE, which has remained poorly characterized.Here we describe the structure of human HYPE, solved by X-ray crystallography, representing the first structure of a eukaryotic FIC-domain protein. We demonstrate that HYPE forms stable dimers with structurally and functionally integrated FIC-domains and with TPR-motifs exposed for protein-protein interactions. As HYPE also uniquely possesses a transmembrane helix, dimerization is likely to affect its positioning and function in the membrane vicinity. The low rate of auto AMPylation of the wild-type HYPE could be due to autoinhibition, consistent with the mechanism proposed for a number of putative FIC AMPylators. Our findings also provide a basis to further consider possible alternative cofactors of HYPE and distinct modes of target-recognition.

摘要

蛋白质腺苷酸化,即AMP从ATP转移至蛋白质靶标,已被确认为某些通常含有FIC结构域的细菌效应蛋白破坏宿主细胞的一种新机制。真核基因组也编码一种FIC结构域蛋白HYPE,其特征仍知之甚少。在此,我们描述了通过X射线晶体学解析的人HYPE的结构,这是真核FIC结构域蛋白的首个结构。我们证明,HYPE形成稳定的二聚体,其FIC结构域在结构和功能上整合在一起,且TPR基序暴露在外用于蛋白质-蛋白质相互作用。由于HYPE还独特地拥有一个跨膜螺旋,二聚化可能会影响其在膜附近的定位和功能。野生型HYPE的自腺苷酸化速率较低可能是由于自抑制作用,这与许多假定的FIC腺苷酰化酶所提出的机制一致。我们的研究结果还为进一步考虑HYPE可能的替代辅因子和不同的靶标识别模式提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5711/4342408/43ae3a5eb4bd/fx1.jpg

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