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内皮素的分子药理学及病理生理学意义

Molecular pharmacology and pathophysiological significance of endothelin.

作者信息

Goto K, Hama H, Kasuya Y

机构信息

Department of Pharmacology, University of Tsukuba, Ibaraki, Japan.

出版信息

Jpn J Pharmacol. 1996 Dec;72(4):261-90. doi: 10.1254/jjp.72.261.

DOI:10.1254/jjp.72.261
PMID:9015736
Abstract

Since the discovery of the most potent vasoconstrictor peptide, endothelin, in 1988, explosive investigations have rapidly clarified much of the basic pharmacological, biochemical and molecular biological features of endothelin, including the presence and structure of isopeptides and their genes (endothelin-1, -2 and -3), regulation of gene expression, intracellular processing, specific endothelin converting enzyme (ECE), receptor subtypes (ETA and ETB), intracellular signal transduction following receptor activation, etc. ECE was recently cloned, and its structure was shown to be a single transmembrane protein with a short intracellular N-terminal and a long extracellular C-terminal that contains the catalytic domain and numerous N-glycosylation sites. In addition to acute contractile or secretory actions, endothelin has been shown to exert long-term proliferative actions on many cell types. In this case, intracellular signal transduction appears to converge to activation of mitogen-activated protein kinase. As a recent dramatic advance, a number of non-peptide and orally active receptor antagonists have been developed. They, as well as current peptide antagonists, markedly accelerated the pace of investigations into the true pathophysiological roles of endogenous endothelin-1 in mature animals; e.g., hypertension, pulmonary hypertension, acute renal failure, cerebral vasospasm, vascular thickening, cardiac hypertrophy, chronic heart failure, etc. Thus, the interference with the endothelin pathway by either ECE-inhibition or receptor blockade may provide an exciting prospect for the development of novel therapeutic drugs.

摘要

自1988年发现最强效的血管收缩肽内皮素以来,大量研究迅速阐明了内皮素的许多基本药理、生化和分子生物学特性,包括异肽及其基因(内皮素-1、-2和-3)的存在与结构、基因表达调控、细胞内加工、特异性内皮素转换酶(ECE)、受体亚型(ETA和ETB)、受体激活后的细胞内信号转导等。ECE最近被克隆,其结构显示为一种单跨膜蛋白,细胞内N端短,细胞外C端长,C端包含催化结构域和多个N-糖基化位点。除了急性收缩或分泌作用外,内皮素还被证明对多种细胞类型具有长期增殖作用。在这种情况下,细胞内信号转导似乎汇聚到丝裂原活化蛋白激酶的激活。作为最近的一项重大进展,已经开发出了多种非肽类且口服有效的受体拮抗剂。它们以及目前的肽类拮抗剂显著加快了对内源性内皮素-1在成熟动物中的真正病理生理作用的研究步伐;例如,高血压、肺动脉高压、急性肾衰竭、脑血管痉挛、血管增厚、心脏肥大、慢性心力衰竭等。因此,通过抑制ECE或阻断受体来干扰内皮素途径可能为新型治疗药物的开发提供令人兴奋的前景。

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1
Molecular pharmacology and pathophysiological significance of endothelin.内皮素的分子药理学及病理生理学意义
Jpn J Pharmacol. 1996 Dec;72(4):261-90. doi: 10.1254/jjp.72.261.
2
Pathophysiology of endothelin in the cardiovascular system.内皮素在心血管系统中的病理生理学
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Endothelin-1 and the regulation of vascular tone.内皮素-1与血管张力的调节
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[New expansion of endothelin research: perspectives for clinical application of endothelin-receptor antagonists].[内皮素研究的新进展:内皮素受体拮抗剂的临床应用前景]
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Endothelin as a regulator of cardiovascular function in health and disease.内皮素作为健康与疾病状态下心血管功能的调节因子。
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Basic and therapeutic relevance of endothelin-mediated regulation.内皮素介导的调节的基础及治疗相关性
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Endothelin receptor antagonists: another potential alternative for cardiovascular diseases.内皮素受体拮抗剂:心血管疾病的另一种潜在替代疗法。
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