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还原型和S-羧甲基化人生长激素:致糖尿病作用的探针

Reduced and S-carboxymethylated human growth hormone: a probe for diabetogenic action.

作者信息

Cameron C M, Kostyo J L, Rillema J A, Gennick S E

出版信息

Am J Physiol. 1984 Nov;247(5 Pt 1):E639-44. doi: 10.1152/ajpendo.1984.247.5.E639.

Abstract

The biological activity profile of reduced and S-carboxymethylated human growth hormone (RCM-hGH) was determined to establish its suitability for study of the diabetogenic property of hGH. RCM-hGH was found to have greatly attenuated in vivo growth-promoting activity in the 9-day weight-gain test in hypophysectomized rats (approximately 1%) and to have a similar low order of in vitro activity in stimulating amino acid incorporation into the protein of the isolated rat diaphragm. RCM-hGH also only had approximately 1% of the in vitro insulin-like activity of the native hormone on isolated adipose tissue from hypophysectomized rats. In contrast, RCM-hGH retained substantial in vivo diabetogenic activity in the ob/ob mouse, appearing to have approximately 50% of the activity of the native hormone. RCM-hGH was also found to retain significant, although attenuated (25%), in vitro lactogenic activity when tested for the ability to stimulate amino acid incorporation into a casein-rich protein fraction in mouse mammary gland explants. Because RCM-hGH exhibits a high degree of diabetogenic activity, although lacking significant anabolic or insulin-like activities, it will be useful as a "monovalent" probe for the study of the molecular mechanism of the diabetogenic action of GH.

摘要

测定还原型和S-羧甲基化人生长激素(RCM-hGH)的生物学活性谱,以确定其是否适合用于研究hGH的致糖尿病特性。在垂体切除大鼠的9天体重增加试验中,发现RCM-hGH的体内促生长活性大幅减弱(约1%),并且在刺激氨基酸掺入分离的大鼠膈肌蛋白质方面,其体外活性也处于相似的低水平。RCM-hGH对垂体切除大鼠分离的脂肪组织的体外胰岛素样活性也仅为天然激素的约1%。相比之下,RCM-hGH在ob/ob小鼠中保留了大量的体内致糖尿病活性,其活性似乎约为天然激素的50%。当检测RCM-hGH刺激氨基酸掺入小鼠乳腺外植体中富含酪蛋白的蛋白质部分的能力时,还发现它保留了显著的(尽管减弱了25%)体外泌乳活性。由于RCM-hGH具有高度的致糖尿病活性,尽管缺乏显著的合成代谢或胰岛素样活性,但它将作为一种“单价”探针,用于研究GH致糖尿病作用的分子机制。

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