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两类抑制Tn10末端反向重复序列中突变的Tn10转座酶突变体。

Two classes of Tn10 transposase mutants that suppress mutations in the Tn10 terminal inverted repeat.

作者信息

Sakai J, Kleckner N

机构信息

Department of Molecular and Cellular Biology, Harvard University, Cambridge, Massachusetts 02138, USA.

出版信息

Genetics. 1996 Nov;144(3):861-70. doi: 10.1093/genetics/144.3.861.

Abstract

Tn10 transposition requires IS10 transposase and essential sequences at the two ends of the element. Mutations in terminal basepairs 6-13 confer particularly strong transposition defects. We describe here the identification of transposase mutations that suppress the transposition defects of such terminus mutations. These mutations are named "SEM" for suppression of ends mutations. All of the SEM mutations suppress more than a single terminus mutation and thus are not simple alterations of transposase/end recognition specificity. The mutations identified fall into two classes on the basis of genetic tests, location within the protein and nature of the amino acid substitution. Class I mutations, which are somewhat allele specific, appear to define a small structural and functional domain of transposase in which hydrophobic interactions are important at an intermediate stage of the transposition reaction, after an effective interaction between the ends but before transposon excision. Class II mutations, which are more general in their effects, occur at a single residue in a small noncritical amino-terminal proteolytic domain of transposase and exert their affects by altering a charge interaction; these mutations may affect act early in the reaction, before or during establishment of an effective interaction between the ends.

摘要

Tn10转座需要IS10转座酶以及该元件两端的必需序列。末端碱基对6 - 13中的突变会导致特别强烈的转座缺陷。我们在此描述了转座酶突变的鉴定,这些突变可抑制此类末端突变的转座缺陷。这些突变因抑制末端突变而被命名为“SEM”。所有的SEM突变都能抑制不止一种末端突变,因此并非是转座酶/末端识别特异性的简单改变。根据遗传测试、在蛋白质中的位置以及氨基酸取代的性质,所鉴定出的突变可分为两类。I类突变在某种程度上具有等位基因特异性,似乎界定了转座酶的一个小的结构和功能域,在转座反应的中间阶段,即在末端之间有效相互作用之后但在转座子切除之前,疏水相互作用在该阶段很重要。II类突变的影响更为普遍,发生在转座酶一个小的非关键氨基末端蛋白水解结构域中的单个残基处,并通过改变电荷相互作用发挥其作用;这些突变可能在反应早期,即在末端之间建立有效相互作用之前或期间起作用。

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