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通过非重叠互补和锌依赖性二聚化揭示莫洛尼鼠白血病病毒整合酶HHCC结构域的功能相互作用。

Functional interactions of the HHCC domain of moloney murine leukemia virus integrase revealed by nonoverlapping complementation and zinc-dependent dimerization.

作者信息

Yang F, Leon O, Greenfield N J, Roth M J

机构信息

Department of Biochemistry, University of Medicine and Dentistry of New Jersey-Robert Wood Johnson Medical School, Piscataway, New Jersey 08854, USA.

出版信息

J Virol. 1999 Mar;73(3):1809-17. doi: 10.1128/JVI.73.3.1809-1817.1999.

Abstract

The retroviral integrase (IN) is required for the integration of viral DNA into the host genome. The N terminus of IN contains an HHCC zinc finger-like motif, which is conserved among all retroviruses. To study the function of the HHCC domain of Moloney murine leukemia virus IN, the first N-terminal 105 residues were expressed independently. This HHCC domain protein is found to complement a completely nonoverlapping construct lacking the HHCC domain for strand transfer, 3' processing and coordinated disintegration reactions, revealing trans interactions among IN domains. The HHCC domain protein binds zinc at a 1:1 ratio and changes its conformation upon binding to zinc. The presence of zinc within the HHCC domain stimulates selective integration processes. Zinc promotes the dimerization of the HHCC domain and protects it from N-ethylmaleimide modification. These studies dissect and define the requirement for the HHCC domain, the exact function of which remains unknown.

摘要

逆转录病毒整合酶(IN)是病毒DNA整合到宿主基因组所必需的。IN的N末端包含一个HHCC锌指样基序,在所有逆转录病毒中都保守。为了研究莫洛尼鼠白血病病毒IN的HHCC结构域的功能,独立表达了最初的N末端105个残基。发现该HHCC结构域蛋白可补充一个完全不重叠的缺乏HHCC结构域的构建体,用于链转移、3'加工和协同解体反应,揭示了IN结构域之间的反式相互作用。HHCC结构域蛋白以1:1的比例结合锌,并在与锌结合时改变其构象。HHCC结构域内锌的存在刺激选择性整合过程。锌促进HHCC结构域的二聚化,并保护其免受N-乙基马来酰亚胺修饰。这些研究剖析并确定了对HHCC结构域的需求,其确切功能仍然未知。

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