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Current state of endothelin receptor antagonism in hypertension and pulmonary hypertension

机译:高血压和肺动脉高压中内皮素受体拮抗作用的现状

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Endothelin 1 (ET-1), a potent vasoconstrictive substance, was discovered in 1988 by Yanagisawa and colleagues, and since then, a quarter of a century has passed. Understanding the biology of ET-1 has rapidly developed by characterizing the components of its receptors and processing enzymes. Numerous studies have revealed not only physiological but also various pathophysiological roles of the ET system. At first, ET-1 was the attractive and promising target for the treatment of hypertension owing to its potent vasoconstrictive nature and a variety of ET receptor antagonists (ERAs) were studied. However, the clinical application to treat hypertension was disappointing because of the side effects, including liver toxicity and fluid retention. On the other hand, ERAs have been established as orphan drugs for the treatment of pulmonary arterial hypertension and improved the prognosis of patients. Furthermore, multipotency of the ET system in the pathogenesis of multiple diseases has led to the development of translational research not only in the field of hypertension but in a variety of fields. Furthermore, a range of studies are ongoing to apply ERAs to clinical situations. In this article, we review the pathophysiological roles of the ET system in hypertension and pulmonary hypertension and the potential of ET receptor antagonism for the treatment of these diseases.
机译:Yanagisawa及其同事于1988年发现了内皮素1(ET-1),这是一种有效的血管收缩物质,从那时起已经过去了25年。通过表征其受体和加工酶的成分,对ET-1生物学的理解迅速发展。大量研究表明,ET系统不仅具有生理作用,还具有多种病理生理作用。首先,由于ET-1具有强大的血管收缩性质,因此它是治疗高血压的诱人且有希望的靶标,并且研究了多种ET受体拮抗剂(ERAs)。但是,由于副作用,包括肝毒性和体液retention留,治疗高血压的临床应用令人失望。另一方面,ERAs已被确定为治疗肺动脉高压并改善患者预后的孤儿药物。此外,ET系统在多种疾病的发病机理中的多能性不仅导致在高血压领域而且在许多领域的转化研究的发展。此外,正在进行将ERA应用于临床的一系列研究。在本文中,我们回顾了ET系统在高血压和肺动脉高压中的病理生理作用,以及ET受体拮抗作用治疗这些疾病的潜力。

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