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结核分枝杆菌核衣壳相关蛋白 HU 和 Lsr2 的物理和功能相互作用:改变 DNA 结合和基因调控。

Physical and functional interaction between nucleoid-associated proteins HU and Lsr2 of Mycobacterium tuberculosis: altered DNA binding and gene regulation.

机构信息

Department of Microbiology and Cell Biology, Indian Institute of Science, C.V. Raman Avenue, Bangalore, 560012, India.

Jawaharlal Nehru Centre for Advanced Scientific Research, Bangalore, 560064, India.

出版信息

Mol Microbiol. 2019 Apr;111(4):981-994. doi: 10.1111/mmi.14202. Epub 2019 Feb 11.

Abstract

Nucleoid-associated proteins (NAPs) in bacteria contribute to key activities such as DNA compaction, chromosome organization and regulation of gene expression. HU and Lsr2 are two principal NAPs in Mycobacterium tuberculosis (Mtb). HU is essential for Mtb survival and is one of the most abundant NAPs. It differs from other eubacterial HU proteins in having a long, flexible lysine- and arginine-rich carboxy-terminal domain. Lsr2 of Mtb is the functional analogue of the bacterial NAP commonly called H-NS. Lsr2 binds to and regulates expression of A/T-rich portions of the otherwise G/C-rich mycobacterial chromosome. Here, we demonstrate that HU and Lsr2 interact to form a complex. The interaction occurs primarily through the flexible carboxy-terminal domain of HU and the acidic amino-terminal domain of Lsr2. The resulting complex, upon binding to DNA, forms thick nucleoprotein rods, in contrast to the DNA bridging seen with Lsr2 and the DNA compaction seen with HU. Furthermore, transcription assays indicate that the HU-Lsr2 complex is a regulator of gene expression. This physical and functional interaction between two NAPs, which has not been reported previously, is likely to be important for DNA organization and gene expression in Mtb and perhaps other bacterial species.

摘要

细菌中的核小体相关蛋白 (NAP) 参与关键活动,如 DNA 紧缩、染色体组织和基因表达调控。HU 和 Lsr2 是结核分枝杆菌 (Mtb) 中的两种主要 NAP。HU 对 Mtb 的生存至关重要,是含量最丰富的 NAP 之一。它与其他真核生物 HU 蛋白的不同之处在于其羧基末端具有长而灵活的赖氨酸和精氨酸丰富结构域。Mtb 的 Lsr2 是通常称为 H-NS 的细菌 NAP 的功能类似物。Lsr2 结合并调节富含 A/T 的部分,否则 Mtb 染色体富含 G/C。在这里,我们证明 HU 和 Lsr2 相互作用形成复合物。这种相互作用主要通过 HU 的柔性羧基末端结构域和 Lsr2 的酸性氨基末端结构域发生。形成的复合物与 DNA 结合后,形成厚的核蛋白棒,与 Lsr2 形成的 DNA 桥和 HU 形成的 DNA 紧缩形成对比。此外,转录分析表明,HU-Lsr2 复合物是基因表达的调节剂。这种两个 NAP 之间以前没有报道过的物理和功能相互作用,可能对 Mtb 甚至其他细菌物种的 DNA 组织和基因表达很重要。

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