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International Union of Pharmacology. XXVIII. Proteinase-Activated Receptors.

机译:国际药理学联合会。二十八。蛋白酶激活的受体。

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Proteinase-activated receptors (PARs) represent a unique subclass of G-protein-coupled receptors of which four family members have now been cloned from a number of species. The novel mechanism of receptor activation involves the proteolytic unmasking of a cryptic N-terminal receptor sequence that, remaining tethered, binds to and triggers receptor function. In addition, short (five to six amino acids) synthetic peptides, based on the proteolytically revealed motif, can activate PARs without the unmasking of the tethered ligand. This article summarizes the experiments leading to the pharmacological characterization and cloning of the four PAR family members and provides a rationale for their designation by the acronym "PAR". The ability to distinguish among the PARs pharmacologically 1) with selective proteinase activators, 2) with receptor-selective peptide agonists, and 3) with peptide and nonpeptide antagonists is discussed, as are the molecular mechanisms of receptor activation and desensitization/internalization. Finally, the potential physiological roles of the PARs, which are widely distributed in many organs in the settings of tissue injury, repair, and remodeling, including embryogenesis and oncogenesis are discussed, and the newly appreciated roles of proteinases as signaling molecules that can act as either functional agonists or antagonists are highlighted.
机译:蛋白酶激活受体(PARs)代表G蛋白偶联受体的独特亚类,现已从许多物种中克隆出其四个家族成员。受体激活的新机制涉及隐性N末端受体序列的蛋白水解作用,该序列在仍被束缚,与受体功能结合并触发受体功能的情况下被揭露。此外,基于蛋白水解揭示的基序的短(5至6个氨基酸)合成肽可以激活PAR,而不会束缚配体。本文概述了导致四个PAR家族成员的药理学表征和克隆的实验,并为使用缩写PAR进行命名提供了理论依据。讨论了药理学上区分PAR的能力:1)使用选择性蛋白酶激活剂,2)使用受体选择性肽激动剂和3)使用肽和非肽拮抗剂,以及受体激活和脱敏/内在化的分子机制。最后,讨论了PARs在组织损伤,修复和重塑中广泛分布在许多器官中的潜在生理学作用,包括胚胎发生和肿瘤发生,以及蛋白酶作为信号分子的新认识作用突出了功能激动剂或拮抗剂。

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