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扩展气溶素家族:从细菌到脊椎动物。

Extending the aerolysin family: from bacteria to vertebrates.

机构信息

Institute of Biochemistry and Biophysics, Polish Academy of Sciences, Warsaw, Poland.

出版信息

PLoS One. 2011;6(6):e20349. doi: 10.1371/journal.pone.0020349. Epub 2011 Jun 8.

Abstract

A number of bacterial virulence factors have been observed to adopt structures similar to that of aerolysin, the principal toxin of Aeromonas species. However, a comprehensive description of architecture and structure of the aerolysin-like superfamily has not been determined. In this study, we define a more compact aerolysin-like domain--or aerolysin fold--and show that this domain is far more widely spread than anticipated since it can be found throughout kingdoms. The aerolysin-fold could be found in very diverse domain and functional contexts, although a toxic function could often be assigned. Due to this diversity, the borders of the superfamily could not be set on a sequence level. As a border-defining member, we therefore chose pXO2-60--a protein from the pathogenic pXO2 plasmid of Bacillus anthracis. This fascinating protein, which harbors a unique ubiquitin-like fold domain at the C-terminus of the aerolysin-domain, nicely illustrates the diversity of the superfamily. Its putative role in the virulence of B. anthracis and its three dimensional model are discussed.

摘要

许多细菌毒力因子被观察到采用类似于气溶素的结构,气溶素是气单胞菌属的主要毒素。然而,尚未确定气溶素样超家族的结构和结构的全面描述。在这项研究中,我们定义了一个更紧凑的气溶素样结构域 - 或气溶素折叠 - 并表明这个结构域比预期的更为广泛,因为它可以在整个生物界中找到。气溶素折叠可以在非常不同的结构域和功能背景下找到,尽管通常可以赋予其毒性功能。由于这种多样性,超级家族的边界不能在序列水平上设置。因此,作为边界定义成员,我们选择了 pXO2-60 - 炭疽杆菌致病 pXO2 质粒中的一种蛋白质。这种引人入胜的蛋白质在气溶素结构域的 C 末端具有独特的泛素样折叠结构域,很好地说明了该超级家族的多样性。讨论了其在炭疽杆菌毒力中的可能作用及其三维模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6d6/3110756/a4cb1323e978/pone.0020349.g001.jpg

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