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首页> 外文期刊>Cell biochemistry and biophysics >G protein-coupled, extracellular Ca2+ (Ca2+(o))-sensing receptor enables Ca2+(o) to function as a versatile extracellular first messenger.
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G protein-coupled, extracellular Ca2+ (Ca2+(o))-sensing receptor enables Ca2+(o) to function as a versatile extracellular first messenger.

机译:G蛋白偶联的细胞外Ca2 +(Ca2 +(o))感应受体使Ca2 +(o)能够充当通用的细胞外第一信使。

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摘要

The cloning of a G protein-coupled, extracellular Ca2+ (Ca2+(o))-sensing receptor (CaR) has afforded a molecular basis for a number of the known effects of Ca2+(o) on tissues involved in maintaining systemic calcium homeostasis, especially parathyroid gland and kidney. In addition to providing molecular tools for showing that CaR messenger RNA and protein are present within these tissues, the cloned CaR has permitted documentation that several human diseases are the result of inactivating or activating mutations of this receptor as well as generation of mice that have targeted disruption of the CaR gene. Characteristic changes in the functions of parathyroid and kidney in these patients as well as in the CaR "knockout" mice have elucidated considerably the CaR's physiological roles in mineral ion homeostasis. Nevertheless, a great deal remains to be learned about how this receptor regulates the functioning of other tissues involved in Ca2+(o) metabolism, such as bone and intestine. Further study of these human diseases and of the mouse models will doubtless be useful in gaining additional understanding of the CaR's roles in these latter tissues. Furthermore, we understand little of the CaR's functions in tissues that are not directly involved in systemic mineral ion metabolism, where the receptor probably serves diverse other roles. Some of these functions may be related to the control of intra- and local extracellular concentrations of Ca2+, while others may be unrelated to either systemic or local ionic homeostasis. In any case, the CaR and conceivably additional receptors/sensors for Ca2+ or other extracellular ions represent versatile regulators of a wide variety of cellular functions and represent important targets for novel classes of therapeutics.
机译:G蛋白偶联的细胞外Ca2 +(Ca2 +(o))感应受体(CaR)的克隆为许多已知的Ca2 +(o)对维持系统钙稳态的组织提供了已知的分子基础。甲状旁腺和肾脏。除了提供显示这些组织内存在CaR信使RNA和蛋白质的分子工具外,克隆的CaR还允许证明某些人类疾病是该受体失活或激活突变的结果,以及靶向产生小鼠的结果CaR基因的破坏。这些患者以及CaR“敲除”小鼠的甲状旁腺和肾脏功能的特征变化已充分阐明了CaR在矿物质离子稳态中的生理作用。然而,关于该受体如何调节与Ca2 +(o)代谢有关的其他组织(如骨骼和肠)的功能,还有很多事情要学习。毫无疑问,对这些人类疾病和小鼠模型的进一步研究将有助于进一步了解CaR在后面这些组织中的作用。此外,我们对不直接参与全身性矿物质离子代谢的组织中的CaR的功能了解甚少,在该组织中,受体可能还发挥着其他多种作用。这些功能中的某些功能可能与控制细胞内和局部Ca2 +的浓度有关,而其他功能可能与全身或局部离子稳态无关。在任何情况下,CaR以及可能的Ca2 +或其他细胞外离子的其他受体/传感器代表了多种细胞功能的多功能调节剂,并代表了新型疗法的重要靶标。

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