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下丘脑的D2受体介导生长抑素-28在多巴胺能刺激下的优先释放。

Hypothalamic D2 receptors mediate the preferential release of somatostatin-28 in response to dopaminergic stimulation.

作者信息

Lewis B M, Dieguez C, Lewis M, Hall R, Scanlon M F

出版信息

Endocrinology. 1986 Oct;119(4):1712-7. doi: 10.1210/endo-119-4-1712.

Abstract

We have studied the effect of dopamine (DA) together with agonist and antagonist drugs of varying specificity on the release of immunoreactive forms of somatostatin (SS) from the perfused, adult rat hypothalamus in vitro. Levels of SS increased from 14.7 +/- 3.7 pg (mean +/- SE) under basal conditions to 137 +/- 23.0 pg after exposure to 10(-6) M DA. This dopaminergic effect was mimicked by the specific D2 agonists bromocriptine (10(-7) M) and LY 171555 (10(-6) M) but not by the D1 agonist SKF 38393A (10(-6) M). The stimulatory action of DA (10(-6) M) was blocked by the active (d) but not the inactive (l) isomer of butaclamol (10(-7) M). Similar blockade was achieved with the specific D2 antagonists metoclopramide (10(-8) M) and domperidone (10(-8) M), whereas the D1 antagonist SCH 23390 partially blocked the stimulation of DA but only when used at X100 greater concentration (10(-6) M). SCH 23390 (10(-8) M) did not affect the dopaminergic stimulation of SS release. HPLC characterization of the immunoreactive forms of SS yielded two peaks which corresponded to SS-28 and SS-14. The ratio of these forms varied significantly under different conditions. In the basal state the ratio of SS-28 to SS-14 was 1:4.4; in response to stimulation with DA, the ratio was 1:1.7 and in response to depolarization with 60 mM K+ the ratio was 1:3.1. In conclusion, the stimulatory action of DA on SS release is mediated via hypothalamic D2 receptors. Furthermore dopaminergic stimulation increases the molar ratio of SS-28 to SS-14 in the total immunoreactive SS which is released.

摘要

我们已经研究了多巴胺(DA)与不同特异性的激动剂和拮抗剂药物共同作用对体外灌流的成年大鼠下丘脑释放免疫反应性生长抑素(SS)的影响。在基础条件下,SS水平从14.7±3.7皮克(平均值±标准误)增加到暴露于10⁻⁶M DA后的137±23.0皮克。这种多巴胺能效应可被特异性D2激动剂溴隐亭(10⁻⁷M)和LY 171555(10⁻⁶M)模拟,但不能被D1激动剂SKF 38393A(10⁻⁶M)模拟。DA(10⁻⁶M)的刺激作用可被布他拉莫的活性(d)异构体(10⁻⁷M)阻断,但不能被无活性的(l)异构体阻断。用特异性D2拮抗剂甲氧氯普胺(10⁻⁸M)和多潘立酮(10⁻⁸M)也能实现类似的阻断,而D1拮抗剂SCH 23390仅在使用浓度高100倍(10⁻⁶M)时部分阻断DA的刺激作用。SCH 23390(10⁻⁸M)不影响多巴胺能对SS释放的刺激作用。对SS免疫反应性形式的HPLC表征产生了两个峰,分别对应于SS - 28和SS - 14。这些形式的比例在不同条件下有显著变化。在基础状态下,SS - 28与SS - 14的比例为1:4.4;对DA刺激的反应中,该比例为1:1.7,对60 mM K⁺去极化的反应中,该比例为1:3.1。总之,DA对SS释放的刺激作用是通过下丘脑D2受体介导的。此外,多巴胺能刺激增加了释放的总免疫反应性SS中SS - 28与SS - 14的摩尔比。

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