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小肠结肠炎耶尔森菌III型分泌注射体形成规则间隔的簇,在激活时会纳入新的机器。

Yersinia enterocolitica type III secretion injectisomes form regularly spaced clusters, which incorporate new machines upon activation.

作者信息

Kudryashev Mikhail, Diepold Andreas, Amstutz Marlise, Armitage Judith P, Stahlberg Henning, Cornelis Guy R

机构信息

Center for Cellular Imaging and NanoAnalytics (C-CINA), Biozentrum, University Basel, WRO-1058, Mattenstrasse 26, Basel, 4058, Switzerland; Focal Area Infection Biology, Biozentrum, University of Basel, Klingelbergstrasse 50/70, Basel, 4056, Switzerland.

出版信息

Mol Microbiol. 2015 Mar;95(5):875-84. doi: 10.1111/mmi.12908. Epub 2015 Jan 30.

Abstract

Bacterial type III secretion systems or injectisomes are multiprotein complexes directly transporting bacterial effector proteins into eukaryotic host cells. To investigate the distribution of injectisomes in the bacterium and the influence of activation of the system on that distribution, we combined in vivo fluorescent imaging and high-resolution in situ visualization of Yersinia enterocolitica injectisomes by cryo-electron tomography. Fluorescence microscopy showed the injectisomes as regularly distributed spots around the bacterial cell. Under secreting conditions (absence of Ca(2+) ), the intensity of single spots significantly increased compared with non-secreting conditions (presence of Ca(2+) ), in line with an overall up-regulation of expression levels of all components. Single injectisomes observed by cryo-electron tomography tended to cluster at distances less than 100 nm, suggesting that the observed fluorescent spots correspond to evenly distributed clusters of injectisomes, rather than single injectisomes. The up-regulation of injectisome components led to an increase in the number of injectisomes per cluster rather than the formation of new clusters. We suggest that injectisome clustering may allow more effective secretion into the host cells.

摘要

细菌III型分泌系统或注射体是将细菌效应蛋白直接转运到真核宿主细胞中的多蛋白复合物。为了研究注射体在细菌中的分布以及该系统的激活对其分布的影响,我们结合了体内荧光成像和通过冷冻电子断层扫描对小肠结肠炎耶尔森菌注射体进行的高分辨率原位可视化。荧光显微镜显示注射体为细菌细胞周围规则分布的斑点。在分泌条件下(无Ca(2+)),与非分泌条件(有Ca(2+))相比,单个斑点的强度显著增加,这与所有组分表达水平的总体上调一致。通过冷冻电子断层扫描观察到的单个注射体倾向于聚集在小于100 nm的距离处,这表明观察到的荧光斑点对应于注射体的均匀分布簇,而不是单个注射体。注射体组分的上调导致每个簇中注射体数量增加,而不是形成新的簇。我们认为注射体聚集可能允许更有效地分泌到宿主细胞中。

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