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耻垢分枝杆菌 Ku 的 C 端低复杂度序列重复调节 DNA 结合。

C-terminal low-complexity sequence repeats of Mycobacterium smegmatis Ku modulate DNA binding.

机构信息

Department of Biological Sciences, Louisiana State University, Baton Rouge, LA 70803, USA.

出版信息

Biosci Rep. 2013 Jan 24;33(1):175-84. doi: 10.1042/BSR20120105.

Abstract

Ku protein is an integral component of the NHEJ (non-homologous end-joining) pathway of DSB (double-strand break) repair. Both eukaryotic and prokaryotic Ku homologues have been characterized and shown to bind DNA ends. A unique feature of Mycobacterium smegmatis Ku is its basic C-terminal tail that contains several lysine-rich low-complexity PAKKA repeats that are absent from homologues encoded by obligate parasitic mycobacteria. Such PAKKA repeats are also characteristic of mycobacterial Hlp (histone-like protein) for which they have been shown to confer the ability to appose DNA ends. Unexpectedly, removal of the lysine-rich extension enhances DNA-binding affinity, but an interaction between DNA and the PAKKA repeats is indicated by the observation that only full-length Ku forms multiple complexes with a short stem-loop-containing DNA previously designed to accommodate only one Ku dimer. The C-terminal extension promotes DNA end-joining by T4 DNA ligase, suggesting that the PAKKA repeats also contribute to efficient end-joining. We suggest that low-complexity lysine-rich sequences have evolved repeatedly to modulate the function of unrelated DNA-binding proteins.

摘要

Ku 蛋白是 DSB(双链断裂)修复中非同源末端连接(NHEJ)途径的一个组成部分。真核生物和原核生物的 Ku 同源物已被鉴定,并显示与 DNA 末端结合。耻垢分枝杆菌 Ku 的一个独特特征是其碱性 C 末端尾部,其中包含几个富含赖氨酸的低复杂度 PAKKA 重复序列,这些重复序列不存在于必需寄生分枝杆菌编码的同源物中。这种 PAKKA 重复序列也是分枝杆菌 Hlp(组蛋白样蛋白)的特征,已经证明它们具有使 DNA 末端并列的能力。出乎意料的是,去除富含赖氨酸的延伸部分增强了 DNA 结合亲和力,但 DNA 与 PAKKA 重复序列之间的相互作用表明,只有全长 Ku 与以前设计仅容纳一个 Ku 二聚体的短茎环含 DNA 形成多个复合物。C 末端延伸促进 T4 DNA 连接酶的 DNA 末端连接,表明 PAKKA 重复序列也有助于有效的末端连接。我们认为,低复杂度富含赖氨酸的序列已经多次进化以调节与无关 DNA 结合蛋白的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9264/3553676/58408e52c59e/bsr2012-0105i001.jpg

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