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Selective and mixed endothelin receptor antagonism in cardiovascular disease.

机译:心血管疾病中的选择性和混合内皮素受体拮抗作用。

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摘要

Within five years of discovering endothelin (ET-1) in 1988, the first report of an orally available ET receptor antagonist was published. Within twelve years, bosentan, the first ET receptor antagonist to gain marketing authorisation, was made available for the treatment of pulmonary artery hypertension (PAH). Since this milestone in ET biology, several ET receptor antagonists have been developed, principally to target cardiovascular disease states. ET-1 acts through two receptors - ET(A) and ET(B). Currently, the mixed antagonist, bosentan, and the selective ET(A) antagonist, sitaxsentan, are both licensed for the treatment of PAH, and clinical trials with these and other agents are ongoing for many diseases, including scleroderma, diabetic nephropathy and prostate cancer. Although there has been no argument about the importance of blocking ET(A) receptors, there remains a long-running debate as to whether additional ET(B) antagonism is of benefit, and this is the topic of the following review.
机译:在1988年发现内皮素(ET-1)的五年内,首次发布了口服ET受体拮抗剂。在十二年内,波生坦,第一个获得市场许可的ET受体拮抗剂,可用于治疗肺动脉高压(PAH)。自从ET生物学这一里程碑式发展以来,已经开发了几种ET受体拮抗剂,主要针对心血管疾病。 ET-1通过两个受体ET(A)和ET(B)起作用。目前,混合拮抗剂波生坦和选择性ET(A)拮抗剂西他生坦均已获许可用于治疗PAH,并且针对这些疾病和其他药物的临床试验正在进行中,包括硬皮病,糖尿病性肾病和前列腺癌。尽管没有关于阻断ET(A)受体的重要性的争论,但关于是否存在额外的ET(B)拮抗作用是否有益仍存在长期争论,这是以下综述的主题。

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