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整合宿主因子增强了由γδ末端赋予的转座免疫。

Integration host factor increases the transpositional immunity conferred by gamma delta ends.

作者信息

Wiater L A, Grindley N D

机构信息

Department of Molecular Biophysics and Biochemistry, Yale University, New Haven, Connecticut 06510.

出版信息

J Bacteriol. 1990 Sep;172(9):4951-8. doi: 10.1128/jb.172.9.4951-4958.1990.

Abstract

The ends of the bacterial transposon gamma delta contain adjacent binding sites for gamma delta transposase and integration host factor (IHF). IHF+ and IHF- strains were used in conjunction with gamma delta transposon ends containing or lacking the site for IHF binding to determine the role that IHF plays in various gamma delta-mediated transposition events. IHF was not essential for the transposition of gamma delta and seemed to decrease its frequency of transposition about threefold. IHF played no role in determining the distribution of gamma delta inserts into a target replicon, nor did it significantly alter the frequency of simple transpositions. The only clear role discerned for IHF and the terminal IHF-binding sites was in transposition immunity. IHF stimulated the immunity of those plasmids that contain an end of gamma delta, provided the end included the terminal IHF-binding site. For both ends, the degree of stimulation of immunity was similar to the stimulation of binding of transposase by IHF.

摘要

细菌转座子γδ的末端含有γδ转座酶和整合宿主因子(IHF)的相邻结合位点。使用IHF+和IHF-菌株,结合含有或缺乏IHF结合位点的γδ转座子末端,以确定IHF在各种γδ介导的转座事件中所起的作用。IHF对于γδ的转座并非必需,并且似乎使其转座频率降低了约三倍。IHF在决定γδ插入靶复制子的分布方面不起作用,也没有显著改变简单转座的频率。对于IHF和末端IHF结合位点而言,唯一明确的作用是在转座免疫方面。如果γδ末端包含末端IHF结合位点,IHF会刺激那些含有γδ末端的质粒的免疫性。对于两个末端,免疫刺激程度与IHF对转座酶结合的刺激程度相似。

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