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在mRNA水平对受体敏感性的调控。

Control of receptor sensitivity at the mRNA level.

作者信息

Morris B J

机构信息

Department of Pharmacology, University of Glasgow, Scotland.

出版信息

Mol Neurobiol. 1993 Fall-Winter;7(3-4):189-205. doi: 10.1007/BF02769175.

Abstract

Neurons are able to adjust the sensitivity of receptor-mediated processes according to the level of receptor activation. Extrapolating from our knowledge of other cellular proteins, regulation of receptor mRNA availability would provide a highly economical means of achieving this objective. Epidermal growth factor is able to induce long-lasting increases in its receptor binding by increasing receptor mRNA levels, and similar effects have been shown for other growth factors. Studies on G-protein-coupled receptors, in particular using adrenoceptor clones transfected into cultured cell lines, have shown that changes in receptor number are generally associated with an alteration in receptor mRNA content. At the neuromuscular junction, dramatic increases in nicotinic acetylcholine receptor number are achieved by activating receptor subunit gene transcription. Less information is available concerning the regulation of ligand-gated ion channels in the brain. Overall, the evidence suggests that receptor mRNA levels are frequently controlled by the degree of receptor stimulation. Receptor mRNA levels are therefore likely to be one of the most important control points for both homologous and heterologous regulation of receptor sensitivity.

摘要

神经元能够根据受体激活水平来调节受体介导过程的敏感性。从我们对其他细胞蛋白的了解推断,调节受体mRNA的可利用性将提供一种实现这一目标的高效经济手段。表皮生长因子能够通过增加受体mRNA水平诱导其受体结合的持久增加,并且其他生长因子也有类似的作用。对G蛋白偶联受体的研究,特别是将肾上腺素能受体克隆转染到培养细胞系中的研究表明,受体数量的变化通常与受体mRNA含量的改变有关。在神经肌肉接头处,通过激活受体亚基基因转录可使烟碱型乙酰胆碱受体数量显著增加。关于大脑中配体门控离子通道的调节,我们所知较少。总体而言,证据表明受体mRNA水平常常受受体刺激程度的控制。因此,受体mRNA水平可能是受体敏感性同源和异源调节的最重要控制点之一。

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