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氮芥诱导的DNA损伤与诱变

DNA damage and mutagenesis induced by nitrogen mustards.

作者信息

Povirk L F, Shuker D E

机构信息

Department of Pharmacology and Toxicology, Medical College of Virginia, Virginia Commonwealth University, Richmond 23298.

出版信息

Mutat Res. 1994 Dec;318(3):205-26. doi: 10.1016/0165-1110(94)90015-9.

Abstract

The nitrogen mustards are bifunctional alkylating agents which, although used extensively in cancer chemotherapy, are themselves highly carcinogenic. All nitrogen mustards induce monofunctional guanine-N7 adducts, as well as interstrand N7-N7 crosslinks involving the two guanines in GNC.GNC (5'-->3'/5'-->3') sequences. In addition, the aromatic mustards melphalan and chlorambucil also induce substantial alkylation at adenine N3, while cyclophosphamide forms phosphotriesters with relatively high frequency. Nitrogen mustards are genotoxic in virtually every assay, and produce a wide array of mutations, including base substitutions at both G.C and A.T base pairs, intragenic as well as multilocus deletions, and chromosomal rearrangements. Mutational spectra generated by these agents in various model systems vary widely, and no single lesion has been implicated as being primarily responsible for mustard-induced mutagenesis. On the contrary, adducts of both adenine and guanine, and monofunctional as well as bifunctional adducts, appear to be involved. Further, it is still not known which types of mutation are responsible for mustard-induced cancers, since no genes have yet been identified which are consistently altered in these malignancies.

摘要

氮芥是双功能烷化剂,尽管在癌症化疗中广泛使用,但它们本身具有高度致癌性。所有氮芥都会诱导单功能鸟嘌呤 - N7加合物,以及涉及GNC.GNC(5'→3'/5'→3')序列中两个鸟嘌呤的链间N7 - N7交联。此外,芳香氮芥美法仑和苯丁酸氮芥也会在腺嘌呤N3处诱导大量烷基化,而环磷酰胺则相对高频地形成磷酸三酯。氮芥在几乎所有检测中都具有遗传毒性,并产生多种突变,包括G.C和A.T碱基对处的碱基替换、基因内以及多位点缺失和染色体重排。这些试剂在各种模型系统中产生的突变谱差异很大,并且没有单一损伤被认为是氮芥诱导诱变的主要原因。相反,腺嘌呤和鸟嘌呤的加合物以及单功能和双功能加合物似乎都参与其中。此外,由于尚未鉴定出在这些恶性肿瘤中持续发生改变的基因,因此仍不清楚哪种类型的突变导致氮芥诱导的癌症。

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