Schiffrin E L
MRC Multidisciplinary Research Group on Hypertension, Clinical Research Institute of Montreal, University of Montreal, Quebec, Canada.
Biol Res. 1998;31(3):199-208.
Endothelins (ET) are 21-aminoacid peptides produced ubiquitously, which were discovered originally as endothelial products. These peptides may play important roles in cardiovascular physiology and pathophysiology. As the pathophysiologic roles of endothelins in cardiovascular disease become increasingly apparent, the potential therapeutic use of endothelin antagonists or endothelin converting enzyme inhibitors is recognized. The main endothelin produced by the endothelium is ET-1. Endothelin-1 is overexpressed in the vascular wall of salt-dependent models of hypertension, such as DOCA-salt hypertensive rats, DOCA-salt-treated spontaneously hypertensive rats (SHR) and Dahl salt-sensitive rats, and in stroke-prone SHR, angiotensin II-infused rats and 1-kidney 1 clip Goldblatt hypertensive rats, but not in SHR, 2-K 1C hypertensive rats or L-NAME-treated rats. The vasoconstrictor effect of ET-1 may contribute to blood pressure elevation and its growth-promoting action to vascular hypertrophy in the hypertensive models which overexpress ET-1 in blood vessels. In rats without generalized activation of the endothelin system, expression of ET-1 is often enhanced in coronary arteries, which suggests a role for ET-1 in myocardial ischemia in hypertension. In rats overexpressing ET-1, ETA/B and ETA-selective antagonists lowered blood pressure slightly, and significantly reduced vascular growth, particularly of small arteries, suggesting that ET-1 has a direct effect on growth. Protection from renal injury and from stroke has also been demonstrated in hypertensive rats treated with endothelin antagonists. In normotensive human subjects endothelin-dependent tone can be shown in the forearm. In a study of mild hypertensive patients, the ETA/B antagonist bosentan reduced blood pressure similarly to an ACE inhibitor. Moderate to severe hypertensive patients presented enhanced expression of ET-1 mRNA in the endothelium of subcutaneous resistance arteries. In blacks with familial hypertension increased plasma levels of endothelin have been found. Thus, ET-1 may play a role in some experimental hypertensive models and in human hypertension. In summary, endothelial ET-1 may be overexpressed in the more severe forms of hypertension, and in certain special populations which may respond particularly well to endothelin antagonism. Endothelin antagonists may prove to be effective disease-modifying agents if in future clinical trials they are shown clinically to blunt vascular growth and endothelial dysfunction, reduce stroke and exert the cardioprotective and renal protective effects already reported in experimental hypertension. These agents could contribute to reduce the long-term complications of hypertension, which remains to be demonstrated in humans.
内皮素(ET)是一种普遍产生的21个氨基酸的肽,最初作为内皮产物被发现。这些肽可能在心血管生理和病理生理中发挥重要作用。随着内皮素在心血管疾病中的病理生理作用越来越明显,内皮素拮抗剂或内皮素转化酶抑制剂的潜在治疗用途得到了认可。内皮细胞产生的主要内皮素是ET-1。在盐依赖性高血压模型的血管壁中,如去氧皮质酮-盐高血压大鼠、去氧皮质酮-盐处理的自发性高血压大鼠(SHR)和 Dahl 盐敏感大鼠,以及在易中风的SHR、输注血管紧张素 II 的大鼠和单肾单夹 Goldblatt 高血压大鼠中,内皮素-1 过度表达,但在SHR、双肾单夹高血压大鼠或L-NAME处理的大鼠中则不然。在血管中过度表达ET-1的高血压模型中,ET-1的血管收缩作用可能导致血压升高,其促生长作用导致血管肥大。在没有内皮素系统普遍激活的大鼠中,冠状动脉中ET-1的表达通常会增强,这表明ET-1在高血压心肌缺血中起作用。在过度表达ET-1的大鼠中,ETA/B和ETA选择性拮抗剂可轻微降低血压,并显著减少血管生长,特别是小动脉的生长,这表明ET-1对生长有直接影响。在用内皮素拮抗剂治疗高血压大鼠中,也已证明对肾损伤和中风有保护作用。在血压正常的人类受试者中,前臂可显示内皮素依赖性张力。在一项轻度高血压患者的研究中,ETA/B拮抗剂波生坦降低血压的效果与ACE抑制剂相似。中度至重度高血压患者皮下阻力动脉内皮中ET-1 mRNA的表达增强。在患有家族性高血压的黑人中,已发现血浆内皮素水平升高。因此,ET-1可能在一些实验性高血压模型和人类高血压中起作用。总之,内皮ET-1可能在更严重的高血压形式以及某些可能对内皮素拮抗作用反应特别良好的特殊人群中过度表达。如果在未来的临床试验中,内皮素拮抗剂在临床上被证明能抑制血管生长和内皮功能障碍、减少中风并发挥已在实验性高血压中报道的心脏保护和肾脏保护作用,那么它们可能被证明是有效的疾病改善药物。这些药物可能有助于减少高血压的长期并发症,这仍有待在人类中得到证实。
