CHROMATIN STRUCTURE, NOT DNA-SEQUENCE SPECIFICITY, IS THE PRIMARY DETERMINANT OF TOPOISOMERASE-II SITES OF ACTION INVIVO

被引：85

作者：

UDVARDY, A

SCHEDL, P

机构：

[1] PRINCETON UNIV, DEPT BIOL, PRINCETON, NJ 08544 USA

[2] HUNGARIAN ACAD SCI, BIOL RES CTR, INST BIOCHEM, H-6701 SZEGED, HUNGARY

来源：

MOLECULAR AND CELLULAR BIOLOGY | 1991年 / 11卷 / 10期

关键词：

D O I：

10.1128/MCB.11.10.4973

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

In the studies reported here we have used topoisomerase II as a model system for analyzing the factors that determine the sites of action for DNA-binding proteins in vivo. To localize topoisomerase II sites in vivo we used an inhibitor of the purified enzyme, the antitumor drug VM-26. This drug stablizes an intermediate in the catalytic cycle, the cleavable complex, and substantially stimulates DNA cleavage by topoisomerase II. We show that lysis of VM-26 treated tissue culture cells with sodium dodecyl sulfate induces highly specific double-strand breaks in genomic DNA, and we present evidence indicating that these double-strand breaks are generated by topoisomerase II. Using indirect end labeling to map the cleavage products, we have examined the in vivo sites of action of topoisomerase II in the 87A7 heat shock locus, the histone repeat, and a tRNA gene cluster at 90BC. Our analysis reveals that chromatin structure, not sequence specificity, is the primary determinant in topoisomerase II site selection in vivo. We suggest that chromatin organization may provide a general mechanism for generating specificity in a wide range of DNA-protein interactions in vivo.

引用

页码：4973 / 4984

页数：12

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