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ABC转运蛋白CvaB的C末端结构域在大肠杆菌素V分泌过程中的核苷酸依赖性二聚化作用。

Nucleotide-dependent dimerization of the C-terminal domain of the ABC transporter CvaB in colicin V secretion.

作者信息

Guo Xiangxue, Harrison Robert W, Tai Phang C

机构信息

Department of Biology, Georgia State University, 24 Peachtree Center Avenue, 402 Kell Hall, Atlanta, GA 30303, USA.

出版信息

J Bacteriol. 2006 Apr;188(7):2383-91. doi: 10.1128/JB.188.7.2383-2391.2006.

Abstract

The cytoplasmic membrane proteins CvaB and CvaA and the outer membrane protein TolC constitute the bacteriocin colicin V secretion system in Escherichia coli. CvaB functions as an ATP-binding cassette transporter, and its C-terminal domain (CTD) contains typical motifs for the nucleotide-binding and Walker A and B sites and the ABC signature motif. To study the role of the CvaB CTD in the secretion of colicin V, a truncated construct of this domain was made and overexpressed. Different forms of the CvaB CTD were found during purification and identified as monomer, dimer, and oligomer forms by gel filtration and protein cross-linking. Nucleotide binding was shown to be critical for CvaB CTD dimerization. Oligomers could be converted to dimers by nucleotide triphosphate-Mg, and nucleotide release from dimers resulted in transient formation of monomers, followed by oligomerization and aggregation. Site-directed mutagenesis showed that the ABC signature motif was involved in the nucleotide-dependent dimerization. The spatial proximity of the Walker A site and the signature motif was shown by disulfide cross-linking a mixture of the A530C and L630C mutant proteins, while the A530C or L630C mutant protein did not dimerize on its own. Taken together, these results indicate that the CvaB CTD formed a nucleotide-dependent head-to-tail dimer.

摘要

细胞质膜蛋白CvaB和CvaA以及外膜蛋白TolC构成了大肠杆菌中细菌素colicin V的分泌系统。CvaB作为一种ATP结合盒转运蛋白发挥作用,其C端结构域(CTD)包含核苷酸结合以及沃克A和B位点的典型基序和ABC特征基序。为了研究CvaB CTD在colicin V分泌中的作用,构建了该结构域的截短体并进行了过表达。在纯化过程中发现了不同形式的CvaB CTD,并通过凝胶过滤和蛋白质交联鉴定为单体、二聚体和寡聚体形式。结果表明核苷酸结合对CvaB CTD二聚化至关重要。寡聚体可通过三磷酸核苷酸 - 镁转化为二聚体,二聚体中核苷酸的释放导致单体的短暂形成,随后发生寡聚化和聚集。定点诱变表明ABC特征基序参与了核苷酸依赖性二聚化。通过对A530C和L630C突变蛋白混合物进行二硫键交联显示了沃克A位点和特征基序的空间接近性,而A530C或L630C突变蛋白自身不会二聚化。综上所述,这些结果表明CvaB CTD形成了一种核苷酸依赖性的头对头二聚体。

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