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The Role of TcdB and TccC Subunits in Secretion of the Photorhabdus Tcd Toxin Complex

机译:TcdB和TccC亚基在Photorhabdus Tcd毒素复合物分泌中的作用。

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摘要

The Toxin Complex (TC) is a large multi-subunit toxin encoded by a range of bacterial pathogens. The best-characterized examples are from the insect pathogens Photorhabdus, Xenorhabdus and Yersinia. They consist of three large protein subunits, designated A, B and C that assemble in a 5∶1∶1 stoichiometry. Oral toxicity to a range of insects means that some have the potential to be developed as pest control technology. The three subunit proteins do not encode any recognisable export sequences and as such little progress has been made in understanding their secretion. We have developed heterologous TC production and secretion models in E. coli and used them to ascribe functions to different domains of the crucial B+C sub-complex. We have determined that the B and C subunits use a secretion mechanism that is either encoded by the proteins themselves or employ an as yet undefined system common to laboratory strains of E. coli. We demonstrate that both the N-terminal domains of the B and C subunits are required for secretion of the whole complex. We propose a model whereby the N-terminus of the C-subunit toxin exports the B+C sub-complex across the inner membrane while that of the B-subunit allows passage across the outer membrane. We also demonstrate that even in the absence of the B-subunit, that the C-subunit can also facilitate secretion of the larger A-subunit. The recognition of this novel export system is likely to be of importance to future protein secretion studies. Finally, the identification of homologues of B and C subunits in diverse bacterial pathogens, including Burkholderia and Pseudomonas, suggests that these toxins are likely to be important in a range of different hosts, including man.
机译:毒素复合物(TC)是由多种细菌病原体编码的大型多亚基毒素。最典型的例子是昆虫病原体Photorhabdus,Xenorhabdus和耶尔森氏菌。它们由三个大的蛋白质亚基组成,分别以5:1:1的化学计量比命名为A,B和C。对多种昆虫的经口毒性意味着其中一些具有作为害虫防治技术的潜力。这三个亚基蛋白不编码任何可识别的输出序列,因此在了解其分泌方面进展甚微。我们已经在大肠杆菌中开发了异源TC生产和分泌模型,并使用它们将功能归因于关键B + C亚复合体的不同域。我们已经确定,B和C亚基使用一种由蛋白质本身编码的分泌机制,或者采用大肠杆菌实验室菌株共有的尚未定义的系统。我们证明,B和C亚基的N末端域都是分泌整个复合物所必需的。我们提出了一个模型,其中C亚基毒素的N末端通过内膜输出B + C亚复合物,而B亚基的复合物则允许穿过外膜。我们还证明,即使在没有B亚基的情况下,C亚基也可以促进更大的A亚基的分泌。这种新颖的出口系统的认可可能对未来的蛋白质分泌研究具有重要意义。最后,鉴定包括伯克霍尔德氏菌和假单胞菌在内的多种细菌病原体中B和C亚基的同源物,表明这些毒素在包括人在内的许多不同宿主中可能很重要。

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