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促甲状腺激素释放激素(TRH)和生长激素释放因子(GRF)通过不同机制刺激生长激素的释放。

TRH and GRF stimulate release of growth hormone through different mechanisms.

作者信息

Szabo M

出版信息

Am J Physiol. 1986 May;250(5 Pt 1):E512-7. doi: 10.1152/ajpendo.1986.250.5.E512.

Abstract

Thyrotropin-releasing hormone (TRH) is an effective stimulator of growth hormone (GH) release from cultured adenohypophysial cells of chronically hypothyroid rats in vitro. The present study explored the question of cAMP and calcium mediation of the GH-stimulatory effect of TRH in this system. A maximally stimulatory concentration of TRH was added together with various concentrations of human GH-releasing factor 40 (hGRF-40) whose action is cAMP mediated, or of dibutyryl cAMP (DBcAMP), to primary monolayer cultures of adenohypophysial cells from thyroidectomized rats. The GH responses to the combined addition of TRH with all doses of GRF or DBcAMP were fully additive, causing parallel elevations of the dose-response curves. Whereas the GH response to maximally effective concentrations of hGRF-40 and DBcAMP, added together, was not greater than that to either secretagogue alone, the inclusion of TRH increased the response to a new Emax. The calcium inhibitors, verapamil, EGTA, and CoCl2, markedly suppressed basal GH release and virtually completely blocked the GH response to TRH, suggesting calcium mediation. In chronically hypothyroid, urethan-anesthetized rats, the in vivo effect of the combined administration of maximally effective doses of TRH and GRF on plasma GH levels was also additive. These findings indicate that TRH stimulates GH release in adenohypophysial cells of hypothyroid rats by a cAMP-independent, calcium-dependent mechanism.

摘要

促甲状腺激素释放激素(TRH)是体外培养的慢性甲状腺功能减退大鼠腺垂体细胞释放生长激素(GH)的有效刺激物。本研究探讨了该系统中TRH对GH刺激作用的cAMP和钙介导问题。将最大刺激浓度的TRH与各种浓度的人生长激素释放因子40(hGRF-40,其作用由cAMP介导)或二丁酰cAMP(DBcAMP)一起添加到甲状腺切除大鼠的腺垂体细胞原代单层培养物中。TRH与所有剂量的GRF或DBcAMP联合添加时的GH反应完全相加,导致剂量反应曲线平行升高。虽然hGRF-40和DBcAMP最大有效浓度一起添加时的GH反应不大于单独使用任何一种促分泌剂时的反应,但加入TRH可使反应增加到新的最大效应(Emax)。钙抑制剂维拉帕米、乙二醇双乙醚二胺四乙酸(EGTA)和氯化钴(CoCl2)显著抑制基础GH释放,并几乎完全阻断对TRH的GH反应,提示钙介导。在慢性甲状腺功能减退、氨基甲酸乙酯麻醉的大鼠中,最大有效剂量的TRH和GRF联合给药对血浆GH水平的体内效应也是相加的。这些发现表明,TRH通过一种不依赖cAMP、依赖钙的机制刺激甲状腺功能减退大鼠腺垂体细胞释放GH。

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