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The androgenic regulation of superhelical-DNA nicking-closing enzyme in rat ventral prostate.

机译:大鼠腹侧前列腺中超螺旋DNA缺口闭合酶的雄激素调节。

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摘要

The activity of superhelical-DNA nicking-closing enzyme (NC enzyme) was measured in nuclei from rat ventral prostate by a fluorimetric assay based on the binding of ethidium bromide to supercoiled phage-PM2 DNA. The nuclear concentration of NC-enzyme activity declined rapidly after castration, although this response could be prevented by daily administration of dihydrotestosterone. The low NC-enzyme activity in involuted prostates (10% of normal) was restored to normal after 8-10 days of treatment with androgen. In the regenerating prostate the time course of restoration of NC-enzyme activity was not in phase with that of DNA synthesis. Examination of nucleosome repeat lengths and the arrangement of nucleosomes along the chromatin fibre revealed no differences in the structural organization of chromatin in prostates with high or low NC-enzyme activity. Together, these results suggest that the major role of NC enzyme is related to the onset and maintenance of differentiation in the prostate and that the activity of this enzyme is not expressed through gross alterations in chromatin structure.
机译:通过基于溴化乙锭与超螺旋噬菌体-PM2 DNA的结合的荧光测定法,在大鼠腹侧前列腺的核中测量了超螺旋DNA缺口闭合酶(NC酶)的活性。去势后,NC酶活性的核浓度迅速下降,尽管这种反应可以通过每天服用二氢睾丸激素来预防。用雄激素治疗8-10天后,被卷入的前列腺中的低NC酶活性(正常值的10%)恢复到正常。在再生前列腺中,NC酶活性恢复的时间过程与DNA合成的时间过程不同。检查核小体重复长度和核小体沿染色质纤维的排列,发现在具有高或低NC酶活性的前列腺中,染色质的结构组织没有差异。总之,这些结果表明,NC酶的主要作用与前列腺分化的开始和维持有关,并且该酶的活性未通过染色质结构的总体改变来表达。

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