Roesch D M, Tian Y, Zheng W, Shi M, Verbalis J G, Sandberg K
Department of Medicine, Georgetown University, Washington, DC 20007, USA.
Endocrinology. 2000 Dec;141(12):4629-36. doi: 10.1210/endo.141.12.7822.
Estrogen replacement therapy significantly reduces the risk of cardiovascular disease in postmenopausal women. Previous studies indicate that estradiol (E2) decreases angiotensin II (AT) receptor density in the adrenal and pituitary in NaCl-loaded rats. We used an in vivo model that eliminates the potentially confounding influence of ACTH to determine whether the E2-induced decrease in adrenal AT receptor expression affects aldosterone responses to angiotensin II (Ang II). Female rats were ovariectomized, treated with oil (OVX) or E2 (OVX+E2; 10 microg, s.c.) for 14 days, and fed a NaCl-deficient diet for the last 7 days to maximize adrenal AT receptor expression and responsiveness. On days 12-14 rats were treated with dexamethasone (DEX; 25 microg, i.p., every 12 h) to suppress plasma ACTH. On day 14 aldosterone secretion was measured after a 30-min infusion of Ang II (330 ng/min). Ang II infusion increased the peak plasma aldosterone levels to a lesser degree in the OVX+E2 than in the OVX rats (OVX, 1870 +/- 290 pg/ml; OVX+E2, 1010 +/- 86 pg/ml; P < 0.05). Ang II-induced ACTH and aldosterone secretion was also studied in rats that were not treated with DEX. In the absence of DEX, the peak plasma aldosterone response was also significantly decreased (OVX, 5360 +/- 1200 pg/ml; OVX+E2, 2960 +/- 570 pg/ml; P < 0.05). However, E2 also reduced the plasma ACTH response to Ang II (P < 0.05; OVX, 220 +/- 29 pg/ml; OVX+E2, 160 +/- 20 pg/ml), suggesting that reduced pituitary ACTH responsiveness to Ang II contributes to the effect of E2 on Ang II-induced aldosterone secretion. Adrenal AT1 binding studies confirmed that E2 significantly reduces adrenal AT1 receptor expression in both the presence and absence of DEX in NaCl-deprived rats. These results indicate that E2-induced decreases in pituitary and adrenal AT1 receptor expression are associated with attenuated pituitary ACTH and adrenal aldosterone responses to Ang II and suggest that estrogen replacement therapy may modulate Ang II-stimulated aldosterone secretion as part of its well known cardioprotective actions.
雌激素替代疗法可显著降低绝经后女性患心血管疾病的风险。先前的研究表明,在高盐饮食的大鼠中,雌二醇(E2)可降低肾上腺和垂体中血管紧张素II(AT)受体的密度。我们使用了一种体内模型,该模型消除了促肾上腺皮质激素(ACTH)的潜在混杂影响,以确定E2诱导的肾上腺AT受体表达降低是否会影响醛固酮对血管紧张素II(Ang II)的反应。将雌性大鼠进行卵巢切除术,分别用橄榄油(OVX组)或E2(OVX+E2组;10微克,皮下注射)处理14天,并在最后7天给予低钠饮食,以最大限度地提高肾上腺AT受体的表达和反应性。在第12至14天,给大鼠腹腔注射地塞米松(DEX;25微克,每12小时一次)以抑制血浆ACTH。在第14天,在输注30分钟的Ang II(330纳克/分钟)后测量醛固酮分泌。与OVX组相比,OVX+E2组中Ang II输注使血浆醛固酮峰值水平升高的程度较小(OVX组,1870±290皮克/毫升;OVX+E2组,1010±86皮克/毫升;P<0.05)。还在未用DEX处理的大鼠中研究了Ang II诱导的ACTH和醛固酮分泌。在没有DEX的情况下,血浆醛固酮峰值反应也显著降低(OVX组,5360±1200皮克/毫升;OVX+E2组,2960±570皮克/毫升;P<0.05)。然而,E2也降低了血浆ACTH对Ang II的反应(P<0.05;OVX组,220±29皮克/毫升;OVX+E2组,160±20皮克/毫升),这表明垂体ACTH对Ang II反应性降低是E2对Ang II诱导的醛固酮分泌产生影响的原因之一。肾上腺AT1结合研究证实,在低钠饮食的大鼠中,无论有无DEX,E2均显著降低肾上腺AT1受体的表达。这些结果表明,E2诱导的垂体和肾上腺AT1受体表达降低与垂体ACTH和肾上腺醛固酮对Ang II的反应减弱有关,提示雌激素替代疗法可能作为其众所周知的心脏保护作用的一部分,调节Ang II刺激的醛固酮分泌。
Zotero 插件