首页> 外文期刊>Clinical neuropharmacology >Lisuride, a dopamine receptor agonist with 5-HT2B receptor antagonist properties: absence of cardiac valvulopathy adverse drug reaction reports supports the concept of a crucial role for 5-HT2B receptor agonism in cardiac valvular fibrosis.
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Lisuride, a dopamine receptor agonist with 5-HT2B receptor antagonist properties: absence of cardiac valvulopathy adverse drug reaction reports supports the concept of a crucial role for 5-HT2B receptor agonism in cardiac valvular fibrosis.

机译:Lisuride是一种具有5-HT2B受体拮抗剂特性的多巴胺受体激动剂:不存在心脏瓣膜病药物不良反应报告支持了在心脏瓣膜纤维化中5-HT2B受体激动作用至关重要的概念。

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OBJECTIVES: The high incidence of fibrotic cardiac valvulopathies reported in association with the 8beta-ergoline dopamine (DA) agonist, pergolide, and also case reports for cabergoline and bromocriptine have made it necessary to review the theoretical basis and actual findings in the case of another DA agonist, the 8alpha-ergoline lisuride (used since the 1970s for migraine prophylaxis as well as since the 1980s for its prolactin-lowering and anti-Parkinson activity). METHODS: We have reviewed the pharmacology of lisuride in relation to other DA agonists, and we have performed a throughout literature search as well as a search of our own and other adverse drug reaction databases for a possible relationship of lisuride with cardiac valvulopathy or for any reports of fibrosis in other locations. RESULTS: Our review of the pharmacology and the literature strongly suggests that drug-induced cardiac valvulopathies are always related to a stimulatory drug effect on trophic 5-HT(2B) receptors. As lisuride isdevoid of such an effect, but on the contrary is an extremely potent 5-HT(2B) antagonist, an association of lisuride therapy with cardiac valvulopathies seems to be highly unlikely. In agreement with this hypothesis, not a single report of a cardiac valvulopathy associated with lisuride therapy has been identified in any database so far.Furthermore, against a background of an estimated 360,000 patient years, we have found only a very small number of cases of any other form of fibrosis (1x retroperitoneal, 2x pleural, 2x pulmonary, 1x interstitial pulmonary changes), in part combined with other risk factors and confounding variables. This closely matches 4 reports available from WHO (1x retroperitoneal, 3x pleural fibrosis). In addition, only 5 other possibly related conditions (3x pleural effusion, 1x pleuritis, 1x pericarditis) were identified in the lisuride adverse drug reaction database of Schering, Berlin. CONCLUSIONS: No link has been found between lisuride use and fibrotic cardiac valvulopathy, in agreement with the 5-HT(2B) receptor antagonist effect of this drug. The very low incidence of spontaneous reports of any other fibrosis could be even compatible with an association by chance in the population exposed to lisuride. Although close monitoring for this kind of side effects is still to be recommended in the therapy with lisuride, our data do not support the concept of a class effect suggesting that all ergot-derived drugs and especially DA receptor agonists with some chemical similarity to the ergot structure will cause or facilitate cardiac valvulopathies as observed with pergolide.
机译:目的:与8β-麦角灵多巴胺(DA)激动剂培高利特有关的纤维化心脏瓣膜病发病率很高,卡麦角林和溴隐亭的病例报告也使得有必要回顾一下另一种情况的理论基础和实际发现DA激动剂8alpha-麦角新碱(自1970年代以来用于预防偏头痛,自1980年代以来一直用于降低催乳激素和抗帕金森氏活性)。方法:我们已经审查了利苏利德与其他DA激动剂的药理关系,并且进行了整篇文献搜索以及我们自己和其他药物不良反应数据库的搜索,以了解利苏利德与心脏瓣膜病或任何与之相关的可能关系其他地方纤维化的报道。结果:我们对药理学和文献的回顾强烈表明,药物诱发的心脏瓣膜病变总是与对营养性5-HT(2B)受体的刺激性药物作用有关。由于瑞舒利特没有这种作用,但是相反地,它是一种非常有效的5-HT(2B)拮抗剂,因此瑞舒利特疗法与心脏瓣膜病的联合似乎非常不可能。与这一假设相符的是,到目前为止,在任何数据库中都没有发现与瑞舒利特治疗相关的心脏瓣膜病的单一报告。此外,在估计360,000患者年的背景下,我们仅发现了极少数病例。任何其他形式的纤维化(1x腹膜后,2x胸膜,2x肺,1x间质性肺变化),部分与其他危险因素和混杂变量结合。这与WHO的4篇报道非常吻合(1x腹膜后,3x胸膜纤维化)。此外,在柏林先灵的异硫脲类药物不良反应数据库中仅发现了其他5种可能相关的疾病(3例胸腔积液,1例胸膜炎,1例心包炎)。结论:在使用lisuride和纤维化心脏瓣膜病之间未发现任何关联,与该药物的5-HT(2B)受体拮抗作用一致。自发报告的任何其他纤维化发生率极低,甚至可能与暴露于异硫脲的人群中的偶然性相关。尽管仍建议在瑞舒利德治疗中建议密切监测此类副作用,但我们的数据并不支持类效应的概念,这表明所有麦角衍生的药物,特别是与麦角有化学相似性的DA受体激动剂如用培高利特所观察到的,这种结构将引起或促进心脏瓣膜病。

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