通过极性募集试验揭示的FtsA亚结构域与后期隔膜形成蛋白之间不依赖Z环的相互作用。
Z-ring-independent interaction between a subdomain of FtsA and late septation proteins as revealed by a polar recruitment assay.
作者信息
Corbin Brian D, Geissler Brett, Sadasivam Mahalakshmi, Margolin William
机构信息
Department of Microbiology and Molecular Genetics, University of Texas Medical School, Houston, TX 77030, USA.
出版信息
J Bacteriol. 2004 Nov;186(22):7736-44. doi: 10.1128/JB.186.22.7736-7744.2004.
Abstract
FtsA, a member of the ATPase superfamily that includes actin and bacterial actin homologs, is essential for cell division of Escherichia coli and is recruited to the Z ring. In turn, recruitment of later essential division proteins to the Z ring is dependent on FtsA. In a polar recruitment assay, we found that FtsA can recruit at least two late proteins, FtsI and FtsN, to the cell poles independently of Z rings. Moreover, a unique structural domain of FtsA, subdomain 1c, which is divergent in the other ATPase superfamily members, is sufficient for this recruitment but not required for the ability of FtsA to localize to Z rings. Surprisingly, targeting the 1c subdomain to the Z ring by fusing it to FtsZ could partially suppress a thermosensitive ftsA mutation. These results suggest that subdomain 1c of FtsA is a completely independent functional domain with an important role in interacting with a septation protein subassembly.
摘要
FtsA是ATP酶超家族的成员之一,该家族包括肌动蛋白和细菌肌动蛋白同源物,它对大肠杆菌的细胞分裂至关重要,并被招募到Z环。反过来,后期重要的分裂蛋白被招募到Z环则依赖于FtsA。在一项极性招募试验中,我们发现FtsA能够独立于Z环将至少两种后期蛋白FtsI和FtsN招募到细胞两极。此外,FtsA的一个独特结构域,即1c亚结构域,在其他ATP酶超家族成员中是不同的,它足以进行这种招募,但对于FtsA定位于Z环的能力并非必需。令人惊讶的是,通过将1c亚结构域与FtsZ融合使其定位于Z环,可部分抑制温度敏感型ftsA突变。这些结果表明,FtsA的1c亚结构域是一个完全独立的功能结构域,在与隔膜蛋白亚组件相互作用中发挥重要作用。
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