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参与DNA从根癌土壤杆菌转移至植物细胞过程的VirB9和VirB10膜蛋白之间的相互作用。

Interactions between VirB9 and VirB10 membrane proteins involved in movement of DNA from Agrobacterium tumefaciens into plant cells.

作者信息

Beaupré C E, Bohne J, Dale E M, Binns A N

机构信息

Plant Sciences Institute, Department of Biology, University of Pennsylvania, Philadelphia 19104-6018, USA.

出版信息

J Bacteriol. 1997 Jan;179(1):78-89. doi: 10.1128/jb.179.1.78-89.1997.

Abstract

The 11 VirB proteins from Agrobacterium tumefaciens are predicted to form a membrane-bound complex that mediates the movement of DNA from the bacterium into plant cells. The studies reported here on the possible VirB protein interactions in such a complex demonstrate that VirB9 and VirB10 can each form high-molecular-weight complexes after treatment with a chemical cross-linker. Analysis of nonpolar virB mutants showed that the formation of the VirB10 complexes does not occur in a virB9 mutant and that VirB9 and VirB10 are not components of the same cross-linked complex. VirB9, when stabilized by the concurrent expression of VirB7, was shown to be sufficient to permit VirB10 to cross-link into its usual high-molecular-weight forms in the absence of other Vir proteins. Randomly introduced single point mutations in virB9 resulted in Agrobacterium strains with severely attenuated virulence. Although some of the mutants contained wild-type levels of VirB9 and displayed an unaltered VirB9 cross-linking pattern, VirB10 cross-linking was drastically reduced. We conclude that specific amino acid residues in VirB9 are necessary for interaction with VirB10 resulting in the capacity of VirB10 to participate in high-molecular-weight complexes that can be visualized by chemical cross-linking.

摘要

根癌土壤杆菌的11种VirB蛋白预计会形成一种膜结合复合物,该复合物介导DNA从细菌转移到植物细胞中。本文报道的关于这种复合物中VirB蛋白可能相互作用的研究表明,在用化学交联剂处理后,VirB9和VirB10各自都能形成高分子量复合物。对非极性virB突变体的分析表明,在virB9突变体中不会形成VirB10复合物,并且VirB9和VirB10不是同一交联复合物的组成部分。当通过同时表达VirB7使VirB9稳定时,结果表明在没有其他Vir蛋白的情况下,VirB9足以使VirB10交联成其通常的高分子量形式。在virB9中随机引入的单点突变导致根癌土壤杆菌菌株的毒力严重减弱。虽然一些突变体含有野生型水平的VirB9并且显示出未改变的VirB9交联模式,但VirB10交联却大幅减少。我们得出结论,VirB9中的特定氨基酸残基对于与VirB10相互作用是必需的,从而导致VirB10能够参与可通过化学交联可视化的高分子量复合物。

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