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原核生物的多细胞性:细菌细胞通讯的纳米孔阵列。

Prokaryotic multicellularity: a nanopore array for bacterial cell communication.

机构信息

Department of Microbiology/Organismic Interactions, University of Tübingen, Tübingen, Germany.

出版信息

FASEB J. 2013 Jun;27(6):2293-300. doi: 10.1096/fj.12-225854. Epub 2013 Feb 26.

Abstract

The transition from unicellular to multicellular life, which occurred several times during evolution, requires tight interaction and communication of neighboring cells. The multicellular cyanobacterium Nostoc punctiforme ATCC 29133 forms filaments of hundreds of interacting cells exchanging metabolites and signal molecules and is able to differentiate specialized cells in response to environmental stimuli. Mutation of cell wall amidase AmiC2 leads to a severe phenotype with formation of aberrant septa in the distorted filaments, which completely lack cell communication and potential for cell differentiation. Here we demonstrate the function of the amidase AmiC2 in formation of cell-joining structures. The AmiC2 protein localizes to the young septum between cells and shows bona fide amidase activity in vivo and in vitro. Vancomycin staining identified the overall septum morphology in living cells. By electron microscopy of isolated peptidoglycan sacculi, the submicroscopic structure of the cell junctions could be visualized, revealing a novel function for a cell wall amidase: AmiC2 drills holes into the cross-walls, forming an array of ~155 nanopores with a diameter of ~20 nm each. These nanopores seem to constitute a framework for cell-joining proteins, penetrating the cell wall. The entire array of junctional nanopores appears as a novel bacterial organelle, establishing multicellularity in a filamentous prokaryote.

摘要

从单细胞到多细胞生命的转变,在进化过程中发生了多次,需要相邻细胞之间的紧密相互作用和通信。多细胞蓝细菌 Nostoc punctiforme ATCC 29133 形成数百个相互作用的细胞的细丝,交换代谢物和信号分子,并能够响应环境刺激分化专门的细胞。细胞壁酰胺酶 AmiC2 的突变导致严重的表型,在扭曲的细丝中形成异常的隔膜,完全缺乏细胞通讯和细胞分化的潜力。在这里,我们证明了酰胺酶 AmiC2 在形成细胞连接结构中的功能。AmiC2 蛋白定位于细胞之间的年轻隔膜上,并在体内和体外显示出真正的酰胺酶活性。万古霉素染色鉴定了活细胞中整个隔膜的形态。通过对分离的肽聚糖囊泡的电子显微镜观察,可以可视化细胞连接处的亚微观结构,揭示了细胞壁酰胺酶的新功能:AmiC2 在细胞壁上打孔,形成一个直径约为 20nm 的约 155 个纳米孔的阵列。这些纳米孔似乎构成了细胞连接蛋白的框架,穿透细胞壁。整个连接纳米孔阵列看起来像一个新的细菌细胞器,在丝状原核生物中建立了多细胞性。

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