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功能和结构表征多聚糖共聚合酶蛋白在依赖于 ATP 结合盒转运蛋白的囊胞生物合成途径中聚合物输出所必需的。

Functional and structural characterization of polysaccharide co-polymerase proteins required for polymer export in ATP-binding cassette transporter-dependent capsule biosynthesis pathways.

机构信息

Department of Molecular and Cellular Biology, University of Guelph, Guelph, Ontario, Canada N1G 2W1.

出版信息

J Biol Chem. 2011 May 13;286(19):16658-68. doi: 10.1074/jbc.M111.228221. Epub 2011 Mar 18.

Abstract

Neisseria meningitidis serogroup B and Escherichia coli K1 bacteria produce a capsular polysaccharide (CPS) that is composed of α2,8-linked polysialic acid (PSA). Biosynthesis of PSA in these bacteria occurs via an ABC (ATP-binding cassette) transporter-dependent pathway. In N. meningitidis, export of PSA to the surface of the bacterium requires two proteins that form an ABC transporter (CtrC and CtrD) and two additional proteins, CtrA and CtrB, that are proposed to form a cell envelope-spanning export complex. CtrA is a member of the outer membrane polysaccharide export (OPX) family of proteins, which are proposed to form a pore to mediate export of CPSs across the outer membrane. CtrB is an inner membrane protein belonging to the polysaccharide co-polymerase (PCP) family. PCP proteins involved in other bacterial polysaccharide assembly systems form structures that extend into the periplasm from the inner membrane. There is currently no structural information available for PCP or OPX proteins involved in an ABC transporter-dependent CPS biosynthesis pathway to support their proposed roles in polysaccharide export. Here, we report cryo-EM images of purified CtrB reconstituted into lipid bilayers. These images contained molecular top and side views of CtrB and showed that it formed a conical oligomer that extended ∼125 Å from the membrane. This structure is consistent with CtrB functioning as a component of an envelope-spanning complex. Cross-complementation of CtrA and CtrB in E. coli mutants with defects in genes encoding the corresponding PCP and OPX proteins show that PCP-OPX pairs require interactions with their cognate partners to export polysaccharide. These experiments add further support for the model of an ABC transporter-PCP-OPX multiprotein complex that functions to export CPS across the cell envelope.

摘要

脑膜炎奈瑟菌 B 群和大肠杆菌 K1 细菌产生一种荚膜多糖(CPS),由α2,8-连接的多聚唾液酸(PSA)组成。这些细菌中 PSA 的生物合成是通过 ABC(ATP 结合盒)转运蛋白依赖性途径进行的。在脑膜炎奈瑟菌中,PSA 向细菌表面的输出需要两种形成 ABC 转运蛋白(CtrC 和 CtrD)的蛋白,以及两种额外的蛋白,CtrA 和 CtrB,它们被提议形成一个跨越细胞包膜的出口复合物。CtrA 是外膜多糖出口(OPX)蛋白家族的成员,该蛋白家族被提议形成一个孔,以介导 CPS 穿过外膜的出口。CtrB 是一种内膜蛋白,属于多糖共聚合酶(PCP)家族。参与其他细菌多糖组装系统的 PCP 蛋白形成从内膜延伸到周质的结构。目前,没有关于参与 ABC 转运蛋白依赖性 CPS 生物合成途径的 PCP 或 OPX 蛋白的结构信息,无法支持它们在多糖输出中的提议作用。在这里,我们报告了纯化的 CtrB 重新构成脂质双层的冷冻电镜图像。这些图像包含了 CtrB 的分子顶视图和侧视图,显示它形成了一个从膜延伸约 125 Å 的锥形寡聚体。该结构与 CtrB 作为包膜延伸复合物的一部分的功能一致。在大肠杆菌突变体中,用编码相应 PCP 和 OPX 蛋白的基因缺陷的基因进行 CtrA 和 CtrB 的交叉互补实验表明,PCP-OPX 对需要与它们的同源伴侣相互作用才能输出多糖。这些实验进一步支持了 ABC 转运蛋白-PCP-OPX 多蛋白复合物的模型,该模型的功能是将 CPS 跨细胞包膜输出。

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