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发现了能够处理 MYXO-CTERM 以及三个具有不变半胱氨酸残基的新型原核 C 末端蛋白分选信号的 myxosortases。

discovery of the myxosortases that process MYXO-CTERM and three novel prokaryotic C-terminal protein-sorting signals that share invariant Cys residues.

机构信息

National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health , Bethesda, Maryland, USA.

出版信息

J Bacteriol. 2024 Jan 25;206(1):e0017323. doi: 10.1128/jb.00173-23. Epub 2023 Dec 12.

Abstract

The LPXTG protein-sorting signal, found in surface proteins of various Gram-positive pathogens, was the founding member of a growing panel of prokaryotic small C-terminal sorting domains. Sortase A cleaves LPXTG, exosortases (XrtA and XrtB) cleave the PEP-CTERM sorting signal, archaeosortase A cleaves PGF-CTERM, and rhombosortase cleaves GlyGly-CTERM domains. Four sorting signal domains without previously known processing proteases are the MYXO-CTERM, JDVT-CTERM, Synerg-CTERM, and CGP-CTERM domains. These exhibit the standard tripartite architecture of a short signature motif, a hydrophobic transmembrane segment, and an Arg-rich cluster. Each has an invariant cysteine in its signature motif. Computational evidence strongly suggests that each of these four Cys-containing sorting signals is processed, at least in part, by a cognate family of glutamic-type intramembrane endopeptidases related to the eukaryotic type II CAAX-processing protease Rce1. For the MYXO-CTERM sorting signals of different lineages, their sorting enzymes, called myxosortases, include MrtX (MXAN_2755 in ), MrtC, and MrtP, all with radically different N-terminal domains but with a conserved core. Related predicted sorting enzymes were also identified for JDVT-CTERM (MrtJ), Synerg-CTERM (MrtS), and CGP-CTERM (MrtA). This work establishes a major new family of protein-sorting housekeeping endopeptidases contributing to the surface attachment of proteins in prokaryotes. IMPORTANCE Homologs of the eukaryotic type II CAAX-box protease Rce1, a membrane-embedded endopeptidase found in yeast and human ER and involved in sorting proteins to their proper cellular locations, are abundant in prokaryotes but not well understood there. This bioinformatics paper identifies several subgroups of the family as cognate endopeptidases for four protein-sorting signals processed by previously unknown machinery. Sorting signals with newly identified processing enzymes include three novel ones, but also MYXO-CTERM, which had been the focus of previous experimental work in the model fruiting and gliding bacterium . The new findings will substantially improve our understanding of Cys-containing C-terminal protein-sorting signals and of protein trafficking generally in bacteria and archaea.

摘要

LPXTG 蛋白分拣信号存在于各种革兰氏阳性病原体的表面蛋白中,是不断增长的原核小分子 C 端分拣结构域家族中的创始成员。Sortase A 切割 LPXTG,外切酶(XrtA 和 XrtB)切割 PEP-CTERM 分拣信号,古菌 Sortase A 切割 PGF-CTERM,菱形蛋白酶切割 GlyGly-CTERM 结构域。四个以前未知的加工蛋白酶的分拣信号结构域是 MYXO-CTERM、JDVT-CTERM、Synerg-CTERM 和 CGP-CTERM 结构域。这些结构域都具有一个短的特征基序、一个疏水性跨膜片段和一个富含精氨酸的簇的标准三分体结构。每个结构域的特征基序中都有一个不变的半胱氨酸。计算证据强烈表明,这四个含半胱氨酸的分拣信号中的每一个都至少部分地被与真核 II 型 CAAX 加工蛋白酶 Rce1 相关的同源家族的谷氨酰胺型跨膜内肽酶加工。对于不同谱系的 MYXO-CTERM 分拣信号,其分拣酶称为 myxosortases,包括 MrtX(MXAN_2755 在 中)、MrtC 和 MrtP,它们都具有截然不同的 N 端结构域,但核心保守。还鉴定了与 JDVT-CTERM(MrtJ)、Synerg-CTERM(MrtS)和 CGP-CTERM(MrtA)相关的预测分拣酶。这项工作确立了一个主要的新的蛋白质分拣管家内肽酶家族,该家族有助于原核生物中蛋白质的表面附着。重要性 真核 II 型 CAAX 盒蛋白酶 Rce1 的同源物是一种存在于酵母和人类内质网中的膜嵌入式内肽酶,参与蛋白质的正确细胞定位分拣,在原核生物中大量存在,但在那里知之甚少。这篇生物信息学论文将该家族的几个亚组鉴定为以前未知机制加工的四个蛋白质分拣信号的同源内切酶。具有新鉴定的加工酶的分拣信号包括三个新的分拣信号,但也包括 MYXO-CTERM,这是以前在模型生殖和滑行细菌 中的实验工作的重点。新的发现将大大提高我们对含半胱氨酸的 C 端蛋白质分拣信号以及细菌和古菌中蛋白质运输的一般理解。

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