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首页> 外文期刊>Current Vascular Pharmacology >Endothelin Receptor Antagonists: A New Therapeutic Option for Improving the Outcome after Solid Organ Transplantation?
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Endothelin Receptor Antagonists: A New Therapeutic Option for Improving the Outcome after Solid Organ Transplantation?

机译:内皮素受体拮抗剂:改善实体器官移植后结果的新治疗选择吗?

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摘要

Initially described as the most potent vasoconstrictor peptide, endothelin (ET) has also been shown to possess extraordinary immunomodulatory and proinflammatory properties. Because of this broad spectrum of biological activities, a possible role of the ET-system in solid organ transplantation has soon become a focus of research. Several studies demonstrated a pathogenetic involvement of ET in ischemia / reperfusion injury of heart, liver, kidney, and lung grafts. ET accumulates during cold storage of organs and can be detected in the effluent preservation solution. In addition ET is very likely to play a pivotal role in the development of chronic rejection, which represents the major cause of late allograft loss. Increased expression of components of the ET-system has been described in areas of neointimal proliferation, a hallmark of chronic graft rejection. Both selective ET-A as well as non-selective ET-A / B receptor antagonists improved histomorphological and functional sequelae of chronic rejection. However these data have largely been derived from experimental animal transplantation, and ET receptor blockers have only recently been introduced in clinical medicine. A significant number of investigational drugs are now being tested in humans, with a main focus on cardiovascular diseases, such as congestive heart failure and pulmonary hypertension. First results have markedly dampened the initial enthusiastic vision of ET receptor blockers being organoprotective super-weapons. Thus the clinical potential of ET antagonists in general, and especially in solid-organ transplantation, is still to be defined.
机译:最初被描述为最有效的血管收缩肽,内皮素(ET)也被证明具有非凡的免疫调节和促炎特性。由于这种广泛的生物活性,ET系统在实体器官移植中的可能作用很快成为研究的焦点。几项研究表明ET致病性参与心脏,肝脏,肾脏和肺移植物的缺血/再灌注损伤。 ET会在器官冷藏期间积聚,并可以在废水保存溶液中检测到。另外,ET很可能在慢性排斥反应的发展中起关键作用,这代表了同种异体移植晚期丢失的主要原因。已经在新内膜增生领域描述了ET系统成分的表达增加,这是慢性移植物排斥的标志。选择性ET-A和非选择性ET-A / B受体拮抗剂均可改善慢性排斥的组织形态和功能后遗症。然而,这些数据主要来自实验动物的移植,并且ET受体阻滞剂直到最近才被引入临床医学。现在,正在对人体进行大量研究性药物的测试,主要关注心血管疾病,例如充血性心力衰竭和肺动脉高压。最初的结果显着抑制了ET受体阻滞剂作为有机保护性超级武器的最初热情。因此,总体上,尤其是在实体器官移植中,ET拮抗剂的临床潜力尚待确定。

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