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来自猪下丘脑的具有促肾上腺皮质激素释放因子活性的高分子量肽。

High molecular weight peptide with corticotropin-releasing factor activity from porcine hypothalami.

作者信息

Schally A V, Chang R C, Arimura A, Redding T W, Fishback J B, Vigh S

出版信息

Proc Natl Acad Sci U S A. 1981 Aug;78(8):5197-201. doi: 10.1073/pnas.78.8.5197.

Abstract

The presence of a corticotropin-releasing factor (CRF) behaving as a peptide with a molecular weight of about 5000 was established after purification of porcine hypothalamic extracts by gel filtration on Sephadex G-25 and then on Sephadex G-50. Purified CRF stimulated the release of corticotropin (ACTH) in three in vitro systems: isolated rat pituitary quarters, monolayer cultures of dispersed pituitary cells, and superfused pituitary cells on a column. A linear logarithmic dose-response relationship existed between 50 and 200 micrograms of CRF preparations per ml and the total amount of ACTH released by the superfused pituitary cells. The pituitary ACTH response to CRF in the pituitary quarters system was also approximately linearly related to the logarithm of the dose of CRF. CRF also stimulated in vivo release of ACTH in rats pretreated with chlorpromazine, morphine, and Nembutal. CRF activity was labile to digestion with trypsin and chymotrypsin and was partially destroyed by pepsin. The evidence indicates that CRF of porcine origin is a polypeptide of a higher molecular weight than previously assumed.

摘要

通过在Sephadex G - 25上,然后在Sephadex G - 50上进行凝胶过滤纯化猪下丘脑提取物后,确定了存在一种分子量约为5000的促肾上腺皮质激素释放因子(CRF)。纯化的CRF在三种体外系统中刺激促肾上腺皮质激素(ACTH)的释放:分离的大鼠垂体四分体、分散垂体细胞的单层培养物以及柱上的灌流垂体细胞。每毫升50至200微克的CRF制剂与灌流垂体细胞释放的ACTH总量之间存在线性对数剂量反应关系。在垂体四分体系统中,垂体对CRF的ACTH反应也与CRF剂量的对数大致呈线性关系。CRF还刺激了用氯丙嗪、吗啡和戊巴比妥预处理的大鼠体内ACTH的释放。CRF活性对胰蛋白酶和糜蛋白酶的消化不稳定,并且被胃蛋白酶部分破坏。证据表明,猪源CRF是一种分子量比先前假设更高的多肽。

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本文引用的文献

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Corticotropin releasing activity of lysine vasopressin analogues.
Endocrinology. 1969 Mar;84(3):579-83. doi: 10.1210/endo-84-3-579.
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Hypothalamic neurohormones regulating anterior pituitary function.调节腺垂体功能的下丘脑神经激素。
Recent Prog Horm Res. 1968;24:497-588. doi: 10.1016/b978-1-4831-9827-9.50016-2.

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