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血管活性肠肽对催乳素分泌的自分泌控制

Autocrine control of prolactin secretion by vasoactive intestinal peptide.

作者信息

Nagy G, Mulchahey J J, Neill J D

机构信息

Department of Physiology and Biophysics, University of Alabama, Birmingham 35294.

出版信息

Endocrinology. 1988 Jan;122(1):364-6. doi: 10.1210/endo-122-1-364.

Abstract

The functions of vasoactive intestinal polypeptide (VIP) and the many other neuropeptides that are localized in the anterior pituitary gland remain unknown although VIP of hypothalamic origin is established to act as a PRL-releasing factor. Evidence is presented here that locally-produced VIP acts in an autocrine fashion to stimulate PRL release. VIP antibodies or a VIP antagonist profoundly but reversibly suppressed PRL secretion in primary cultures of rat pituitary cells or the GH3 cell line. This evidence was obtained with the use of a reverse hemolytic plaque assay for microscopic demonstration of PRL release from individual cells under conditions precluding cell-cell interaction. We suggest that most of the high rate of "spontaneous" PRL secretion attributed to lactotropes deprived of hypothalamic influence is due in fact to the stimulatory effects of VIP acting in an autocrine fashion.

摘要

血管活性肠肽(VIP)以及定位于垂体前叶的许多其他神经肽的功能仍不清楚,尽管已经确定下丘脑来源的VIP可作为催乳素释放因子。本文提供的证据表明,局部产生的VIP以自分泌方式刺激催乳素释放。VIP抗体或VIP拮抗剂可显著但可逆地抑制大鼠垂体细胞原代培养物或GH3细胞系中的催乳素分泌。该证据是通过反向溶血空斑试验获得的,用于在排除细胞间相互作用的条件下显微镜下显示单个细胞释放催乳素。我们认为,大多数归因于缺乏下丘脑影响的催乳细胞的“自发性”催乳素高分泌率实际上是由于VIP以自分泌方式发挥的刺激作用。

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