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甲状旁腺激素的蛋白激酶-C激活结构域。

The protein kinase-C activation domain of the parathyroid hormone.

作者信息

Jouishomme H, Whitfield J F, Chakravarthy B, Durkin J P, Gagnon L, Isaacs R J, MacLean S, Neugebauer W, Willick G, Rixon R H

机构信息

Institute for Biological Sciences, National Research Council of Canada, Ottawa, Ontario.

出版信息

Endocrinology. 1992 Jan;130(1):53-60. doi: 10.1210/endo.130.1.1727720.

Abstract

The PTH activates both adenylate cyclase and a mechanism that increases membrane-associated protein kinase-C (PKC) activity. To define the hormone's PKC activation domain we have used a panel of PTH fragments and ROS 17/2 rat osteosarcoma cells as the target cells. PTH equally and maximally increased PKC activity in ROS 17/2 cell membranes at physiological concentrations between 1-50 pM and 5-50 nM, but not at intermediate concentrations or concentrations above 50 nM. The PKC-stimulating picomolar concentrations of PTH did not stimulate adenylate cyclase in ROS 17/2 cells, while the PKC-stimulating nanomolar concentrations of the hormone did stimulate adenylate cyclase, with an EC50 of 1-2 nM. Very high concentrations of PTH, such as 100 nM, that did not increase membrane PKC activity were still able to maximally stimulate adenylate cyclase. PTH fragments lacking the N-terminal amino acids needed for adenylate cyclase activation increased membrane PKC activity, and the PKC activation domain was found to lie within the 28-34 region of the PTH molecule. This was confirmed by showing that optimally effective picomolar concentrations of the human PTH-(28-34) fragment itself were able to increase membrane-associated PKC activity to the same extent as the optimally effective picomolar concentrations of the intact PTH-(1-84) or the larger PTH-(1-34) or PTH-(3-34) fragments.

摘要

甲状旁腺激素(PTH)可激活腺苷酸环化酶以及一种能增加膜相关蛋白激酶C(PKC)活性的机制。为了确定该激素的PKC激活结构域,我们使用了一组PTH片段,并以ROS 17/2大鼠骨肉瘤细胞作为靶细胞。在1 - 50 pM和5 - 50 nM的生理浓度下,PTH能同等程度且最大程度地增加ROS 17/2细胞膜中的PKC活性,但在中间浓度或高于50 nM的浓度下则不能。能刺激PKC的皮摩尔浓度的PTH不会刺激ROS 17/2细胞中的腺苷酸环化酶,而能刺激PKC的纳摩尔浓度的该激素则会刺激腺苷酸环化酶,其半数有效浓度(EC50)为1 - 2 nM。非常高浓度的PTH,如100 nM,虽不会增加膜PKC活性,但仍能最大程度地刺激腺苷酸环化酶。缺乏激活腺苷酸环化酶所需N端氨基酸的PTH片段会增加膜PKC活性,并且发现PKC激活结构域位于PTH分子的28 - 34区域内。通过表明人PTH - (28 - 34)片段本身的最佳有效皮摩尔浓度能够将膜相关PKC活性增加到与完整的PTH - (1 - 84)或更大的PTH - (1 - 34)或PTH - (3 - 34)片段的最佳有效皮摩尔浓度相同的程度,这一点得到了证实。

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