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钙在促肾上腺皮质激素释放因子介导的促肾上腺皮质激素释放机制中的作用。

The role of calcium in the mechanism of corticotropin releasing factor mediated ACTH release.

作者信息

Sobel D O

出版信息

Peptides. 1986 May-Jun;7(3):443-8. doi: 10.1016/0196-9781(86)90012-4.

Abstract

To investigate the role of calcium (Ca+2) in CRF stimulated ACTH release, we studied the effect of the following conditions on CRF (10 nM) mediated ACTH release in primary pituitary monolayer culture: different concentrations of Ca+2; EGTA; lanthanum (La+3) and nifedipine, blockers of calcium cell influx and penfluridol, trifluoperazine, and pimozide, inhibitors of calmodulin activation. Higher concentrations of Ca+2 in the culture medium led to greater amounts of CRF induced ACTH release. EGTA at 3 mM decreased the amount of CRF stimulated ACTH release by 60% but did not alter the spontaneous release of ACTH. At 0.5 mM and 1.0 mM La+3, ACTH release induced by CRF was inhibited by 23% and 35% respectively (p less than 0.01). Nifedipine (both 10(-5) and 10(-4) M) inhibited CRF stimulated ACTH release but only to a maximum of 30%. This inhibition was completely overcome by the addition of 12 mM calcium. Penfluridol, pimozide, and trifluoperazine blocked the release of ACTH induced by CRF by 63%, 26%, and 0% respectively. In conclusion, extracellular Ca+2, Ca+2 influx, and calmodulin play a role in the mechanism of CRF stimulated ACTH in vitro.

摘要

为研究钙(Ca+2)在促肾上腺皮质激素释放因子(CRF)刺激促肾上腺皮质激素(ACTH)释放中的作用,我们在原代垂体单层培养中研究了以下条件对CRF(10 nM)介导的ACTH释放的影响:不同浓度的Ca+2;乙二醇双四乙酸(EGTA);镧(La+3)和硝苯地平,钙细胞内流阻滞剂以及五氟利多、三氟拉嗪和匹莫齐特,钙调蛋白激活抑制剂。培养基中较高浓度的Ca+2导致CRF诱导的ACTH释放量增加。3 mM的EGTA使CRF刺激的ACTH释放量减少60%,但不改变ACTH的自发释放。在0.5 mM和1.0 mM的La+3时,CRF诱导的ACTH释放分别被抑制23%和35%(p<0.01)。硝苯地平(10^(-5) M和10^(-4) M)均抑制CRF刺激的ACTH释放,但最大抑制率仅为30%。加入12 mM钙可完全克服这种抑制作用。五氟利多、匹莫齐特和三氟拉嗪分别使CRF诱导的ACTH释放量减少63%、26%和0%。总之,细胞外Ca+2、Ca+2内流和钙调蛋白在体外CRF刺激ACTH释放的机制中发挥作用。

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