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2-乙酰氨基芴、2-氨基芴和N-羟基-2-乙酰氨基芴在体内和体外与大鼠肝细胞核DNA及蛋白质的共价结合。

Covalent binding of 2-acetylaminofluorene, 2-aminofluorene, and N-hydroxy-2-acetylaminofluorene to rat liver nuclear DNA and protein in vivo and in vitro.

作者信息

Stout D L, Hemminki K, Becker F F

出版信息

Cancer Res. 1980 Oct;40(10):3579-84.

PMID:7438044
Abstract

Binding of the hepatocarcinogen 2-acetylaminofluorene (AAF) and two metabolites, 2-aminofluorene (AF) and N-hydroxy-2-acetylaminofluorene (N-OH-AAF), to the DNA and protein of rat hepatic nuclei was examined in vitro and in a cell-free system. Three and one-half hr following a single injection of each compound in equimolar amounts. DNA contained approximately 50% more of the compounds per mg than did protein. The amount of N-OH-AAF bound to DNA was 4 times greater than that of AAF, while AF bound in intermediate amounts. When incubated with nuclei in a cell-free system, AAF seldom bound in measurable amounts, while significant amounts of N-OH-AAF and AF bound to both DNA and protein. As occurred in vivo, DNA bound more of each per mg than did protein. The amount of N-OH-AFF bound to intranuclear DNA increased 54% when an aliquot of the postmicrosomal liver fraction was added to the incubation mixture, but maximum binding of AF occurred in the absence of any other liver fraction. Thus, it was shown that two AAF metabolites, AF and N-OH-AAF, bind covalently to the DNA and protein of hepatic nuclei more readily than does AAF itself and that binding in a cell-free system parallels binding in vivo. Additional evidence suggests that rat hepatic nuclei are capable of mediating the binding of AF and N-OH-AAF to macromolecules through distinct enzyme systems. This is the first demonstration that the nucleus is capable of metabolizing AF to an electrophile that can bind covalently to DNA.

摘要

在体外和无细胞体系中检测了肝癌致癌物2-乙酰氨基芴(AAF)及其两种代谢产物2-氨基芴(AF)和N-羟基-2-乙酰氨基芴(N-OH-AAF)与大鼠肝细胞核DNA和蛋白质的结合情况。以等摩尔量单次注射每种化合物后3.5小时,DNA每毫克所含的化合物比蛋白质多约50%。与DNA结合的N-OH-AAF的量是AAF的4倍,而AF的结合量处于中间水平。当在无细胞体系中与细胞核一起孵育时,AAF很少以可测量的量结合,而大量的N-OH-AAF和AF与DNA和蛋白质都有结合。正如在体内发生的那样,DNA每毫克结合的每种化合物都比蛋白质多。当将一份微粒体后肝脏组分加入孵育混合物中时,与核内DNA结合的N-OH-AFF的量增加了54%,但AF在没有任何其他肝脏组分的情况下结合量最大。因此,研究表明,AAF的两种代谢产物AF和N-OH-AAF比AAF本身更容易与肝细胞核的DNA和蛋白质共价结合,并且在无细胞体系中的结合与体内结合情况相似。其他证据表明,大鼠肝细胞核能够通过不同的酶系统介导AF和N-OH-AAF与大分子的结合。这是首次证明细胞核能够将AF代谢为一种可与DNA共价结合的亲电试剂。

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