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类固醇受体与核基质的相互作用。DNA的作用。

Steroid receptor-nuclear matrix interactions. The role of DNA.

作者信息

Buttyan R, Olsson C A, Sheard B, Kallos J

出版信息

J Biol Chem. 1983 Dec 10;258(23):14366-70.

PMID:6643487
Abstract

The interaction of sex steroid hormone receptors with the nuclear matrix (NM) of target and non-target tissue was investigated using a simple in vitro binding assay. Steroid receptors can recognize acceptor sites on the NM of target cells; androgen receptor binds with the highest apparent affinity to rat prostate NM; similarly estrogen receptor binds with the highest apparent affinity to uterine NM. Furthermore, the steroid receptor-NM interaction depends upon the hormonal status of the animal. The binding of androgen receptor to rat prostate NM was drastically reduced upon hormone withdrawal (castration) and fully recovered upon hormonal stimulation. When NM were prepared by an alternate method (DNase I digestion prior to high salt extraction) known to digest "active" chromatin, no preferential receptor binding to target tissue NM was observed. Although the NM fraction contains less than 1% of the total nuclear DNA, the matrix-associated DNA sequences seem to be, at least in part, responsible for specific receptor recognition. DNA extracted from the prostate NM was shown to be a potent competitor for androgen receptor binding as measured by DNA-cellulose competition experiments. Moreover, this DNA recognition also depends upon the hormonal status of the animal. These studies are consistent with the notion that hormonal manipulation induces changes in the NM-associated DNA sequences of steroid hormone target tissue.

摘要

利用一种简单的体外结合试验,研究了性甾体激素受体与靶组织和非靶组织的核基质(NM)之间的相互作用。甾体激素受体能够识别靶细胞核基质上的受体位点;雄激素受体与大鼠前列腺核基质的结合具有最高的表观亲和力;同样,雌激素受体与子宫核基质的结合具有最高的表观亲和力。此外,甾体激素受体与核基质的相互作用取决于动物的激素状态。激素撤除(去势)后,雄激素受体与大鼠前列腺核基质的结合急剧减少,而激素刺激后则完全恢复。当通过另一种已知可消化“活性”染色质的方法(在高盐提取之前进行DNase I消化)制备核基质时,未观察到受体与靶组织核基质的优先结合。尽管核基质部分占总核DNA的比例不到1%,但与核基质相关的DNA序列似乎至少部分地负责特异性受体识别。通过DNA纤维素竞争实验测量,从前列腺核基质中提取的DNA被证明是雄激素受体结合的有效竞争者。此外,这种DNA识别也取决于动物的激素状态。这些研究与激素操纵诱导甾体激素靶组织中与核基质相关的DNA序列发生变化的观点一致。

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