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氮芥对含有C-C错配碱基对的DNA双链进行异常交联。

Anomalous cross-linking by mechlorethamine of DNA duplexes containing C-C mismatch pairs.

作者信息

Romero R M, Mitas M, Haworth I S

机构信息

Department of Biochemistry and Molecular Biology and Pharmaceutical Sciences, University of Southern California, 1985 Zonal Avenue, Los Angeles, California 90033, USA.

出版信息

Biochemistry. 1999 Mar 23;38(12):3641-8. doi: 10.1021/bi981935j.

Abstract

Nitrogen mustards such as mechlorethamine have previously been shown to covalently cross-link DNA through the N7 position of the two guanine bases of a d[GXC].d[GYC] duplex sequence, a so-called 1,3 G-G-cross-link, when X-Y = C-G or T-A. Here, we report the formation of a new mechlorethamine cross-link with the d[GXC].d[GYC] fragment when X-Y is a C-C mismatch pair. Mechlorethamine cross-links this fragment preferentially between the two mismatched cytosine bases, rather than between the guanine bases. The cross-link also forms when one or both of the guanine bases of the d[GCC].d[GCC] fragment are replaced by N7-deazaguanine, and, more generally, forms with any C-C mismatch, regardless of the flanking base pairs. Piperidine cleavage of the cross-link species containing the d[GCC].d[GCC] sequence gives DNA fragments consistent with alkylation at the mismatched cytosine bases. We also provide evidence that the cross-link reaction occurs between the N3 atoms of the two cytosine bases by showing that the formation of the C-C cross-link is pH dependent for both mechlorethamine and chlorambucil. Dimethyl sulfate (DMS) probing of the cross-linked d[GCC].d[GCC] fragment showed that the major groove of the guanine adjacent to the C-C mismatch is still accessible to DMS. In contrast, the known minor groove binder Hoechst 33258 inhibits the cross-link formation with a C-C mismatch pair flanked by A-T base pairs. These results suggest that the C-C mismatch is cross-linked by mechlorethamine in the minor groove. Since C-C pairs may be involved in unusual secondary structures formed by the trinucleotide repeat sequence d[CCG]n, and associated with triplet repeat expansion diseases, mechlorethamine may serve as a useful probe for these structures.

摘要

诸如氮芥之类的氮芥类药物先前已被证明,当X-Y = C-G或T-A时,可通过d[GXC].d[GYC]双链体序列中两个鸟嘌呤碱基的N7位置与DNA共价交联,即所谓的1,3 G-G交联。在此,我们报告当X-Y为C-C错配碱基对时,氮芥与d[GXC].d[GYC]片段形成了一种新的交联。氮芥优先在两个错配的胞嘧啶碱基之间交联该片段,而非在鸟嘌呤碱基之间。当d[GCC].d[GCC]片段中的一个或两个鸟嘌呤碱基被N7-脱氮鸟嘌呤取代时,也会形成这种交联,更普遍地说,任何C-C错配都会形成这种交联,而与侧翼碱基对无关。含有d[GCC].d[GCC]序列的交联物种经哌啶裂解后产生的DNA片段与在错配的胞嘧啶碱基处发生烷基化一致。我们还提供证据表明,两个胞嘧啶碱基的N3原子之间会发生交联反应,因为无论是氮芥还是苯丁酸氮芥,C-C交联的形成都依赖于pH值。对交联的d[GCC].d[GCC]片段进行硫酸二甲酯(DMS)探测表明,与C-C错配相邻的鸟嘌呤的大沟仍可被DMS接近。相比之下,已知的小沟结合剂Hoechst 33258可抑制与两侧为A-T碱基对的C-C错配碱基对形成交联。这些结果表明,C-C错配是由氮芥在小沟中交联的。由于C-C碱基对可能参与由三核苷酸重复序列d[CCG]n形成的异常二级结构,并与三联体重复扩增疾病相关,因此氮芥可能是这些结构的有用探针。

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