Binding of 5-bromouracil-containing S/MAR DNA to the nuclear matrix.

H. Ogino, M. Fujii, W. Satou, Toshikazu Suzuki, E. Michishita, D. Ayusawa
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引用次数: 20

Abstract

Substitution of thymine with 5-bromouracil in DNA is known to change interaction between DNA and proteins, thereby inducing various biological phenomena. We hypothesize that A/T-rich scaffold/nuclear matrix attachment region (S/MAR) sequences are involved in the effects of 5-bromodeoxyuridine. We examined an interaction between DNA containing an intronic S/MAR sequence of the immunoglobulin heavy chain gene and nuclear halos prepared from HeLa cells. Upon substitution with 5-bromouracil, the S/MAR DNA bound more tightly to the nuclear halos. The multi-functional nuclear matrix protein YY1 was also found to bind more strongly to 5-bromouracil-substituted DNA containing its recognition motif. These results are consistent with the above hypothesis.
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含5-溴酸的S/MAR DNA与核基质的结合。
已知胸腺嘧啶在DNA中被5-溴酸取代会改变DNA与蛋白质之间的相互作用,从而诱发各种生物现象。我们推测富含A/ t的支架/核基质附着区(S/MAR)序列参与了5-溴脱氧尿苷的作用。我们检测了含有免疫球蛋白重链基因内含子S/MAR序列的DNA与HeLa细胞制备的核晕之间的相互作用。与5-溴醛酸取代后,S/MAR DNA与核晕结合更紧密。多功能核基质蛋白YY1也被发现与含有其识别基序的5-溴酰取代的DNA结合更强。这些结果与上述假设一致。
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