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将人类免疫缺陷病毒1整合酶束缚于一个DNA位点可引导整合至附近序列。

Tethering human immunodeficiency virus 1 integrase to a DNA site directs integration to nearby sequences.

作者信息

Bushman F D

机构信息

Salk Institute for Biological Studies, La Jolla, CA 92037.

出版信息

Proc Natl Acad Sci U S A. 1994 Sep 27;91(20):9233-7. doi: 10.1073/pnas.91.20.9233.

Abstract

Certain retrovirus and retrotransposons display strong biases in the selection of host DNA sites for integration. To probe the possibility that simple tethering of the retroelement integrase protein to a target DNA site is sufficient to direct integration, the activities of a hybrid composed of human immunodeficiency virus 1 integrase and lambda repressor were analyzed. In in vitro reactions containing several target DNAs, the lambda repressor-integrase hybrid was found to direct integration selectively to targets containing lambda operators. Addition of lambda repressor blocked selective integration, indicating that binding to the operators was required. The lambda repressor-integrase hybrid protein directed integration primarily to sites near the operators on the same face of the B-DNA helix, indicating that target DNA was probably captured by looping out the intervening sequences. Such hybrid integrase proteins may be useful for directing retroviral integration to specific sequences in vivo.

摘要

某些逆转录病毒和逆转座子在选择整合的宿主DNA位点时表现出强烈的偏好。为了探究将逆转元件整合酶蛋白简单地与目标DNA位点相连是否足以指导整合,对由人类免疫缺陷病毒1整合酶和λ阻遏物组成的杂交体的活性进行了分析。在含有几种目标DNA的体外反应中,发现λ阻遏物-整合酶杂交体将整合选择性地导向含有λ操纵基因的目标。添加λ阻遏物可阻断选择性整合,这表明与操纵基因的结合是必需的。λ阻遏物-整合酶杂交蛋白主要将整合导向B-DNA螺旋同一面上靠近操纵基因的位点,这表明目标DNA可能是通过环出中间序列而被捕获的。这种杂交整合酶蛋白可能有助于在体内将逆转录病毒整合导向特定序列。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f487/44786/39e4e2bafaf5/pnas01142-0047-a.jpg

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