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内皮素-1与血管张力的调节

Endothelin-1 and the regulation of vascular tone.

作者信息

La M, Reid J J

机构信息

Department of Medical Laboratory Science, Royal Melbourne Institute of Technology, Victoria, Australia.

出版信息

Clin Exp Pharmacol Physiol. 1995 May;22(5):315-23. doi: 10.1111/j.1440-1681.1995.tb02008.x.

Abstract
  1. In 1988, Yanagisawa et al. reported the presence of a potent peptide from the supernatant of porcine endothelial cells. This was later named endothelin-1 (ET-1) and was found to belong to a new family of vasoconstrictor peptides. There are at least three isoforms of endothelin: ET-1, endothelin-2 and endothelin-3. 2. ET-1 is produced from a larger precursor molecule by endothelin converting enzyme (ECE); there may be a number of ECE but the most physiologically relevant appears to be a membrane-bound neutral metalloprotease. The endothelin precursor is produced on demand and is regulated at the mRNA level. 3. Two subtypes of mammalian endothelin receptors have been cloned and sequenced: ETA receptors which mediate vasoconstriction and ETB receptors which mediate both vasoconstriction and vasodilatation. However, functional studies have indicated that other subtypes of endothelin receptors may exist. 4. ET-1 has a wide range of biological actions apart from its direct effects on vascular tone, including constriction of non-vascular smooth muscle, cardiac effects, mitogenesis and stimulation of the release of hormones such as atrial natriuretic peptide and prostacyclin. At low concentrations which have no direct vasoconstrictor action, ET-1 potentiates the effect of other vasoconstrictor agonists. 5. The precise role of ET-1 in health and disease is not well defined at present; however, there are indications that it may have a role in the pathogenesis of some cardiovascular disease states, including subarachnoid haemorrhage, renal ischaemia and certain types of hypertension.
摘要
  1. 1988年,柳泽等人报道了从猪内皮细胞上清液中发现一种强效肽。该肽后来被命名为内皮素-1(ET-1),并被发现属于一个新的血管收缩肽家族。内皮素至少有三种亚型:ET-1、内皮素-2和内皮素-3。2. ET-1由内皮素转换酶(ECE)从一个较大的前体分子产生;可能有多种ECE,但生理上最相关的似乎是一种膜结合中性金属蛋白酶。内皮素前体按需产生,并在mRNA水平受到调节。3. 已克隆并测序了两种哺乳动物内皮素受体亚型:介导血管收缩的ETA受体和介导血管收缩及血管舒张的ETB受体。然而,功能研究表明可能存在其他内皮素受体亚型。4. 除了对血管张力的直接影响外,ET-1还有广泛的生物学作用,包括非血管平滑肌收缩、心脏效应、有丝分裂以及刺激心房利钠肽和前列环素等激素的释放。在无直接血管收缩作用的低浓度下,ET-1可增强其他血管收缩激动剂的作用。5. 目前ET-1在健康和疾病中的精确作用尚不清楚;然而,有迹象表明它可能在某些心血管疾病状态的发病机制中起作用,包括蛛网膜下腔出血、肾缺血和某些类型的高血压。

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