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脑内血管紧张素Ⅱ受体亚型与雌性大鼠促黄体生成素和催乳素分泌的调控。

Brain Angiotensin II Receptor Subtypes and the Control of Luteinizing Hormone and Prolactin Secretion in Female Rats.

机构信息

Department of Physiology, University of California, San Francisco, California 94143-0444, USA.

出版信息

J Neuroendocrinol. 1992 Aug;4(4):441-7. doi: 10.1111/j.1365-2826.1992.tb00191.x.

DOI:10.1111/j.1365-2826.1992.tb00191.x
PMID:21554628
Abstract

The present experiments examined the role of the two recently identified angiotensin II (Ang II) receptor subtypes, AT, and AT(2) , in the central nervous system regulation of luteinizing hormone (LH) and prolactin secretion in estrogen- and progesterone-treated ovariectomized rats. In this animal model, intracerebroventricular (icv) injection of Ang II stimulates LH and inhibits prolactin release. The specific Ang II receptor subtype antagonists losartan (AT(1) ) or PD123177 (AT(2) ) were administered (icv) in various doses (10 ng to 1,000 ng) 10 min prior to icv injection of Ang II (100 ng). Control animals were pretreated with artificial cerebrospinal fluid prior to Ang II administration. Blood samples for LH and prolactin determinations were taken from conscious, freely-moving rats prior to and following injection of the antagonists and Ang II. Water intake was measured. Ang ll-induced water intake was attenuated 62% by 1,000 ng losartan; water intake was not affected by lower doses of losartan or by any dose of PD123177. Ang ll-induced stimulation of LH release was abolished by the 1,000 ng doses of losartan and PD123177 and attenuated by the 500 ng doses of both drugs. Lower doses did not affect Ang ll-induced LH secretion. Ang ll-induced inhibition of prolactin release was significantly reduced by the 1,000 ng doses of both losartan and PD123177. Lower doses of either drug did not affect the Ang II inhibition of prolactin release. Previous studies had shown that Ang II administration into the anterior hypothalamus-medial preoptic (AHPO) area stimulated LH release. This brain area contains AT(1) receptors. To investigate the potential brain site where the AT(2) receptor may influence LH release, Ang II was injected into the locus ceruleus, a brain nucleus which contains predominately the AT(2) receptor subtype. Ang II administration into the locus ceruleus was paired with an injection of artificial cerebrospinal fluid or Ang II into the AHPO area. Injection of Ang II into the AHPO area stimulated LH release. Injection into the locus ceruleus did not affect LH secretion, nor did it modify the rise in LH elicited by administration of Ang II into the AHPO area. Plasma levels of prolactin were not altered by any of these injections. Taken together, these data demonstrate that, in estrogen- and progesterone-treated female rats, icv Ang ll-induced water intake is mediated by the AT, receptor subtype, while Ang ll-induced changes in LH and prolactin secretion appear to be mediated by both the AT(2) and AT(2) receptor subtypes. The latter observations are one of the first suggesting a potential function for the AT(2) subtype in vivo, although the physiological relevance of this observation, as well as the site of action for the effects on LH and prolactin, remain to be established.

摘要

本实验研究了两种最近发现的血管紧张素 II (Ang II) 受体亚型 AT 和 AT(2) 在中枢神经系统对雌激素和孕激素处理的去卵巢大鼠促黄体激素 (LH) 和催乳素分泌的调节作用。在这种动物模型中,脑室内 (icv) 注射 Ang II 刺激 LH 并抑制催乳素释放。特异性 Ang II 受体亚型拮抗剂 losartan (AT(1) ) 或 PD123177 (AT(2) ) 以不同剂量 (10ng 至 1000ng) 在 icv 注射 Ang II (100ng) 前 10 分钟给药 (icv)。在给予 Ang II 之前,对照动物用人工脑脊液进行预处理。在注射拮抗剂和 Ang II 前后,从意识清醒、自由活动的大鼠中抽取血液样本,用于测定 LH 和催乳素。测量水的摄入量。1000ng losartan 可使 Ang ll 诱导的水摄入量减少 62%;较低剂量的 losartan 或任何剂量的 PD123177 均不影响水的摄入量。1000ng 的 losartan 和 PD123177 可消除 Ang ll 诱导的 LH 释放刺激,而两种药物的 500ng 剂量可减弱 Ang ll 诱导的 LH 分泌。较低剂量不影响 Ang ll 诱导的 LH 分泌。1000ng 的 losartan 和 PD123177 均可显著减少 Ang ll 诱导的催乳素释放抑制。两种药物的较低剂量均不影响 Ang II 对催乳素释放的抑制作用。先前的研究表明,将 Ang II 注入下丘脑前区-中脑前视前区 (AHPO) 区域会刺激 LH 释放。该脑区包含 AT(1) 受体。为了研究 AT(2) 受体可能影响 LH 释放的潜在脑区,将 Ang II 注入蓝斑核,这是一个主要包含 AT(2) 受体亚型的脑核。将 Ang II 注入蓝斑核与将人工脑脊液或 Ang II 注入 AHPO 区域同时进行。将 Ang II 注入 AHPO 区域会刺激 LH 释放。将 Ang II 注入蓝斑核不会影响 LH 分泌,也不会改变注入 AHPO 区域的 Ang II 引起的 LH 升高。这些注射均未改变催乳素的血浆水平。综上所述,这些数据表明,在雌激素和孕激素处理的雌性大鼠中,icv Ang II 诱导的水摄入量是由 AT 受体亚型介导的,而 Ang II 诱导的 LH 和催乳素分泌变化似乎同时由 AT(2) 和 AT(2) 受体亚型介导。后一种观察结果是第一个提示 AT(2) 亚型在体内可能具有潜在功能的观察结果之一,尽管这种观察结果的生理相关性以及对 LH 和催乳素的作用部位仍有待确定。

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