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[应用³H-环磷酰胺后大鼠肝脏染色质烷基化的研究——“精细分布”与动力学]

[Investigation of alkylation in rat liver chromatin after application of 3H-cyclophosphamid--"fine-distribution" and kinetics].

作者信息

Harbers E, Warnecke P, Hollandt H, Kruse K

出版信息

Z Krebsforsch Klin Onkol Cancer Res Clin Oncol. 1977;88(3):237-54. doi: 10.1007/BF00305362.

Abstract

The alkylation of chromatin constituents (DNA, histones and non-histones) in liver cell nuclei was investigated at various times after intraperitoneal injection of rats with 3H-cyclophosphamid. The highest alkylation was found in the DNA, the lowest in the histones; the euchromatic portions were alkylated several times higher compared to those of the heterochromatin. The eventual elimination of 3H-activity with time indicates that cyclophosphamid leads to repair processes in the DNA, this conclusion being supported by other experimental observations. In some of the 16 subfractions of the nonhistone proteins, alkylated portions are apparantly eliminated by normal protein turnover; however, in other nonhistones this elimination is inhibited, whereby in one subfraction it seems to be accelerated. The results of analog experiments with 14C-tryptophan as a precursor for nonhistone protein synthesis serve as a reference for this. In supplementary in-vitro model experiments using triaziquon as an alkylating agent indications for DNA-Protein-cross-links in chromatin could be obtained by the technique of X-ray low angle scattering, and according to sedimentation behaviour.

摘要

在给大鼠腹腔注射³H-环磷酰胺后的不同时间,研究了肝细胞细胞核中染色质成分(DNA、组蛋白和非组蛋白)的烷基化情况。发现DNA的烷基化程度最高,组蛋白的最低;常染色质部分的烷基化程度比异染色质部分高几倍。随着时间的推移³H活性的最终消除表明环磷酰胺导致了DNA的修复过程,这一结论得到了其他实验观察结果的支持。在非组蛋白的16个亚组分中,一些亚组分中的烷基化部分显然通过正常的蛋白质周转而消除;然而,在其他非组蛋白中,这种消除受到抑制,其中一个亚组分中的消除似乎被加速。以¹⁴C-色氨酸作为非组蛋白蛋白质合成前体的类似实验结果为此提供了参考。在使用三嗪醌作为烷基化剂的补充体外模型实验中,通过X射线小角散射技术并根据沉降行为,可以获得染色质中DNA-蛋白质交联的迹象。

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