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低剂量持续暴露于雌二醇对雌激素受体(I型)和核II型位点的影响。

The effect of low dose continuous exposure to estradiol on the estrogen receptor (type I) and nuclear type II sites.

作者信息

Markaverich B M, Roberts R R, Alejandro M, Clark J H

出版信息

Endocrinology. 1984 Mar;114(3):814-20. doi: 10.1210/endo-114-3-814.

Abstract

These studies were done to evaluate the temporal relationships between cytoplasmic and nuclear estrogen receptors (type I sites), nuclear type II estrogen binding sites, and uterotropic response (true uterine growth; DNA content) after low dose estrogen administration to adult-ovariectomized rats by beeswax pellet implant. Administration of low dose (2.5 micrograms estradiol-17 beta/pellet) estrogen pellets resulted in a slight accumulation of nuclear type I sites (approximately 1700 sites per cell above ovariectomized controls) and a 2-fold stimulation of nuclear type II estrogen binding sites (approximately 5,000 sites per cell) at short times (1-24 h) after estrogen treatment. By 96 h, nuclear levels of type I sites were not different from control even though nuclear type II sites remained elevated and uterotropic response was maintained. Similar temporal responses were observed after treatment with a higher dose estradiol (20 micrograms/pellet) except that early response (1-24 h) to the hormone was accompanied by a more pronounced accumulation (approximately 3,000 sites per cell above control) of type I sites in the nucleus. By 96 h after the administration of the 20-micrograms estradiol pellet, nuclear type I sites declined to control, however nuclear type II sites continued to increase (approximately 30,000 sites per cell) and maximum uterotropic response was observed. Comparison of the results obtained with these two dose levels of estradiol suggested that at early times (1-24 h) after treatment only a very small quantity (approximately 1,700 sites per cell) of nuclear type I sites is required for uterine growth. Likewise, although nuclear type II sites can be maximally stimulated (approximately 30,000 sites per cell) by higher doses of estrogen (20 micrograms) only 5,000 sites per cell may be necessary for maximal response. Surprisingly, uterine growth was sustained by very low to non-measurable quantities of type I sites in the nucleus (96 h). Regardless of the initial numbers of type I sites translocated to the nucleus (approximately 1,700 sites per cell, 2.5 micrograms estradiol; approximately 3,000 sites per cell, 20 micrograms estradiol), at early times (1-24 h), these levels decline to control approximately 96 h after treatment. These results are not due to a decreased rate of estrogen release from the beeswax pellet implant and the data suggest a down-regulation of nuclear type I sites is a normal response to the hormone under these experimental conditions, even though maximum uterine growth is maintained.

摘要

这些研究旨在评估成年去卵巢大鼠经蜂蜡丸植入给予低剂量雌激素后,细胞质和细胞核雌激素受体(I型位点)、细胞核II型雌激素结合位点与子宫促生长反应(真正的子宫生长;DNA含量)之间的时间关系。给予低剂量(每丸含2.5微克雌二醇-17β)雌激素丸后,在雌激素处理后的短时间内(1 - 24小时),细胞核I型位点略有积累(比去卵巢对照组每细胞约多1700个位点),细胞核II型雌激素结合位点增加了2倍(每细胞约5000个位点)。到96小时时,尽管细胞核II型位点仍然升高且子宫促生长反应得以维持,但细胞核I型位点的水平与对照组无异。用更高剂量的雌二醇(每丸含20微克)处理后观察到类似的时间反应,只是对该激素的早期反应(1 - 24小时)伴随着细胞核中I型位点更明显的积累(比对照组每细胞约多3000个位点)。在给予20微克雌二醇丸96小时后,细胞核I型位点降至对照组水平,然而细胞核II型位点继续增加(每细胞约30000个位点)并观察到最大的子宫促生长反应。对这两种雌二醇剂量水平获得的结果进行比较表明,在处理后的早期(1 - 24小时),子宫生长仅需要极少量(每细胞约1700个位点)的细胞核I型位点。同样,尽管更高剂量的雌激素(20微克)可使细胞核II型位点受到最大刺激(每细胞约30000个位点),但最大反应可能仅需要每细胞5000个位点。令人惊讶的是,细胞核中极低至不可测量数量的I型位点(96小时)就能维持子宫生长。无论转运至细胞核的I型位点初始数量如何(每细胞约1700个位点,2.5微克雌二醇;每细胞约3000个位点,20微克雌二醇),在早期(1 - 24小时),这些水平在处理后约96小时降至对照组水平。这些结果并非由于蜂蜡丸植入物中雌激素释放速率降低,数据表明在这些实验条件下,细胞核I型位点的下调是对该激素的正常反应,即使最大子宫生长得以维持。

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