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SmeA是一种小膜蛋白,在链霉菌孢子形成过程中具有多种功能,包括将一种SpoIIIE/FtsK样蛋白靶向细胞分裂隔膜。

SmeA, a small membrane protein with multiple functions in Streptomyces sporulation including targeting of a SpoIIIE/FtsK-like protein to cell division septa.

作者信息

Ausmees Nora, Wahlstedt Helene, Bagchi Sonchita, Elliot Marie A, Buttner Mark J, Flärdh Klas

机构信息

Department of Cell and Molecular Biology, Uppsala University, BMC Box 596, 75124, Uppsala, Sweden.

出版信息

Mol Microbiol. 2007 Sep;65(6):1458-73. doi: 10.1111/j.1365-2958.2007.05877.x.

DOI:10.1111/j.1365-2958.2007.05877.x
PMID:17824926
Abstract

Sporulation in aerial hyphae of Streptomyces coelicolor involves profound changes in regulation of fundamental morphogenetic and cell cycle processes to convert the filamentous and multinucleoid cells to small unigenomic spores. Here, a novel sporulation locus consisting of smeA (encoding a small putative membrane protein) and sffA (encoding a SpoIIIE/FtsK-family protein) is characterized. Deletion of smeA-sffA gave rise to pleiotropic effects on spore maturation, and influenced the segregation of chromosomes and placement of septa during sporulation. Both smeA and sffA were expressed specifically in apical cells of sporogenic aerial hyphae simultaneously with or slightly after Z-ring assembly. The presence of smeA-like genes in streptomycete chromosomes, plasmids and transposons, often paired with a gene for a SpoIIIE/FtsK- or Tra-like protein, indicates that SmeA and SffA functions might be related to DNA transfer. During spore development SffA accumulated specifically at sporulation septa where it colocalized with FtsK. However, sffA did not show redundancy with ftsK, and SffA function appeared distinct from the DNA translocase activity displayed by FtsK during closure of sporulation septa. The septal localization of SffA was dependent on SmeA, suggesting that SmeA may act as an assembly factor for SffA and possibly other proteins required during spore maturation.

摘要

天蓝色链霉菌气生菌丝中的孢子形成涉及到基本形态发生和细胞周期调控过程的深刻变化,从而将丝状多核细胞转化为小的单基因组孢子。在此,对一个由smeA(编码一种假定的小膜蛋白)和sffA(编码一种SpoIIIE/FtsK家族蛋白)组成的新型孢子形成位点进行了表征。缺失smeA-sffA对孢子成熟产生多效性影响,并影响孢子形成过程中染色体的分离和隔膜的定位。smeA和sffA在产孢气生菌丝的顶端细胞中与Z环组装同时或稍晚特异性表达。链霉菌染色体、质粒和转座子中存在类似smeA的基因,通常与一个SpoIIIE/FtsK或Tra样蛋白的基因配对,这表明SmeA和SffA的功能可能与DNA转移有关。在孢子发育过程中,SffA特异性地聚集在孢子形成隔膜处,与FtsK共定位。然而,sffA与ftsK没有显示出冗余性,并且SffA的功能似乎不同于FtsK在孢子形成隔膜关闭期间显示的DNA转位酶活性。SffA的隔膜定位依赖于SmeA,这表明SmeA可能作为SffA以及孢子成熟过程中可能需要的其他蛋白质的组装因子。

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