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丝状噬菌体 IKe 感染的结构和能量基础。

Structural and energetic basis of infection by the filamentous bacteriophage IKe.

机构信息

Laboratorium für Biochemie and Bayreuther Zentrum für Molekulare Biowissenschaften, Universität Bayreuth, D-95440 Bayreuth, Germany.

出版信息

Mol Microbiol. 2012 Jun;84(6):1124-38. doi: 10.1111/j.1365-2958.2012.08079.x. Epub 2012 May 17.

Abstract

Filamentous phage use the two N-terminal domains of their gene-3-proteins to initiate infection of Escherichia coli. One domain interacts with a pilus, and then the other domain binds to TolA at the cell surface. In phage fd, these two domains are tightly associated with each other, which renders the phage robust but non-infectious, because the TolA binding site is inaccessible. Activation for infection requires partial unfolding, domain disassembly and prolyl isomerization. Phage IKe infects E. coli less efficiently than phage fd. Unlike in phage fd, the pilus- and TolA-binding domains of phage IKe are independent of each other in stability and folding. The site for TolA binding is thus always accessible, but the affinity is very low. The structures of the two domains, analysed by X-ray crystallography and by NMR spectroscopy, revealed a unique fold for the N-pilus-binding domain and a conserved fold for the TolA-binding domain. The absence of an activation mechanism as in phage fd and the low affinity for TolA probably explain the low infectivity of phage IKe. They also explain why, in a previous co-evolution experiment with a mixture of phage fd and phage IKe, all hybrid phage adopted the superior infection mechanism of phage fd.

摘要

丝状噬菌体使用其基因 3 蛋白的两个 N 端结构域来启动对大肠杆菌的感染。其中一个结构域与菌毛相互作用,然后另一个结构域与细胞表面的 TolA 结合。在噬菌体 fd 中,这两个结构域紧密相关,这使得噬菌体具有很强的稳定性但不能感染,因为 TolA 结合位点无法接触。感染的激活需要部分展开、结构域解体和脯氨酸异构化。噬菌体 IKe 对大肠杆菌的感染效率低于噬菌体 fd。与噬菌体 fd 不同,噬菌体 IKe 的菌毛和 TolA 结合结构域在稳定性和折叠方面是相互独立的。因此,TolA 的结合位点始终可以接触,但亲和力非常低。通过 X 射线晶体学和 NMR 光谱分析这两个结构域的结构,揭示了 N 菌毛结合结构域的独特折叠和 TolA 结合结构域的保守折叠。缺乏像噬菌体 fd 那样的激活机制以及与 TolA 的低亲和力可能解释了噬菌体 IKe 低感染力的原因。它们还解释了为什么在之前与噬菌体 fd 和噬菌体 IKe 的混合物进行的共同进化实验中,所有杂交噬菌体都采用了噬菌体 fd 的优越感染机制。

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