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链霉菌的气生发育需要天冬酰胺酰基内肽酶活性。

Aerial development in Streptomyces coelicolor requires sortase activity.

机构信息

Department of Biology and Institute for Infectious Disease Research, McMaster University, 1280 Main Street West, Hamilton, Ontario, Canada.

出版信息

Mol Microbiol. 2012 Mar;83(5):992-1005. doi: 10.1111/j.1365-2958.2012.07983.x. Epub 2012 Feb 8.

DOI:10.1111/j.1365-2958.2012.07983.x
PMID:22296345
Abstract

Streptomyces coelicolor is a multicellular bacterium whose life cycle encompasses three differentiated states: vegetative hyphae, aerial hyphae and spores. Among the factors required for aerial development are the 'chaplins', a family of eight secreted proteins that coat the surface of aerial hyphae. Three chaplins (the 'long' chaplins, ChpA, B and C) possess an LAXTG-containing C-terminal sorting signal and are predicted sortase substrates. The five remaining 'short' chaplins are presumed to be associated with the cell surface through interactions with the long chaplins. We show here that two sortase enzymes, SrtE1 and SrtE2, cleave LAXTG-containing peptides at two distinct positions in vitro, and are required for cell wall anchoring of ChpC in vivo. srtE1/E2 double mutants are delayed in aerial hyphae formation, do not sporulate and fail to display all short chaplins on their aerial surfaces. Surprisingly, these mutant characteristics were not shared by a long chaplin mutant, which exhibited only modest delays in aerial development, leading us to revise the current model of chaplin-mediated aerial development. The sortase mutant phenotype, instead, appears to stem from an inability to transcribe aerial hyphae-specific genes, whose products have diverse functions. This suggests that sortase activity triggers an important, and previously unknown, developmental checkpoint.

摘要

变铅青链霉菌是一种多细胞细菌,其生命周期包括三种分化状态:营养菌丝、气生菌丝和孢子。气生发育所需的因素包括“查plin”,这是一类覆盖气生菌丝表面的八种分泌蛋白。三个“长”查plin(ChpA、B 和 C)具有含有 LAXTG 的 C 末端分拣信号,并且被预测为 sortase 底物。其余的五个“短”查plin 被认为通过与长查plin的相互作用与细胞表面相关联。我们在这里表明,两种 sortase 酶 SrtE1 和 SrtE2 在体外切割含有 LAXTG 的肽在两个不同的位置,并在体内需要 ChpC 的细胞壁锚定。srtE1/E2 双突变体在气生菌丝形成中延迟,不产孢,并且不在其气生表面上显示所有短查plin。令人惊讶的是,这些突变体特征并未被长查plin突变体共享,该突变体仅在气生发育中表现出适度的延迟,这导致我们修正了查plin 介导的气生发育的当前模型。相反,sortase 突变体表型似乎源于无法转录气生菌丝特异性基因,其产物具有多种功能。这表明 sortase 活性触发了一个重要的、以前未知的发育检查点。

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