Clozapine-induced Myocarditis: Pathophysiologic Mechanisms and Implications for Therapeutic Approaches.

IF 2.4 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Simon W Rabkin, Jacky K K Tang
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引用次数: 1

Abstract

Clozapine, a superior treatment for treatment-resistant schizophrenia can cause potentially life-threatening myocarditis and dilated cardiomyopathy. While the occurrence of this condition is well known, its molecular mechanisms are unclear and may be multifactorial. Putative mechanisms warrant an in-depth review not only from the perspective of toxicity but also for understanding the molecular mechanisms of the adverse cardiac effects of clozapine and the development of novel therapeutic approaches. Clozapine-induced cardiac toxicity encompasses a diverse set of pathways, including (i) immune modulation and proinflammatory processes encompassing an IgEmediated (type I hypersensitivity) response and perhaps a cytokine release syndrome (ii) catecholaminergic activation (iii) induction of free radicals and oxidative stress (iv) activation of cardiomyocyte cell death pathways, including apoptosis, ischemia through impairment in coronary blood flow via changes in endothelial production of NO and vasoconstriction induced by norepinephrine as well as other factors released from cardiac mast cells. (v) In addition, an extensive examination of the effects of clozapine on non-cardiac cellular proteins demonstrates that clozapine can impair enzymes involved in cellular metabolism, such as pyruvate kinase, mitochondrial malate dehydrogenase, and other proteins, including α-enolase, triosephosphate isomerase and cofilin, which might explain clozapine-induced reductions in myocardial energy generation for cell viability as well as contractile function. Pharmacologic antagonism of these cellular protein effects may lead to the development of strategies to antagonize the cardiac damage induced by clozapine.

氯氮平诱导的心肌炎:病理生理机制和治疗方法的意义。
氯氮平,一种治疗难治性精神分裂症的优越疗法,可能导致潜在的危及生命的心肌炎和扩张性心肌病。虽然这种情况的发生是众所周知的,但其分子机制尚不清楚,可能是多因素的。假设的机制不仅需要从毒性的角度进行深入的审查,而且还需要了解氯氮平对心脏不良反应的分子机制和开发新的治疗方法。氯氮平诱导的心脏毒性包括多种途径,包括(i)免疫调节和促炎过程,包括ig介导的(i型超敏反应)反应,可能还有细胞因子释放综合征(ii)儿茶酚胺能激活(iii)自由基和氧化应激的诱导(iv)心肌细胞死亡途径的激活,包括细胞凋亡。心肌肥大细胞释放的去甲肾上腺素和其他因子引起的血管收缩,通过内皮细胞一氧化氮生成的改变和冠状动脉血流损伤引起的缺血。(v)此外,对氯氮平对非心脏细胞蛋白质的影响的广泛研究表明,氯氮平可损害细胞代谢所涉及的酶,如丙酮酸激酶、线粒体苹果酸脱氢酶和其他蛋白质,包括α-烯醇化酶、三磷酸异构酶和cofilin,这可能解释了氯氮平引起的心肌能量产生的减少,以促进细胞活力和收缩功能。这些细胞蛋白作用的药理学拮抗作用可能导致拮抗氯氮平引起的心脏损伤的策略的发展。
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来源期刊
Current molecular pharmacology
Current molecular pharmacology Pharmacology, Toxicology and Pharmaceutics-Drug Discovery
CiteScore
4.90
自引率
3.70%
发文量
112
期刊介绍: Current Molecular Pharmacology aims to publish the latest developments in cellular and molecular pharmacology with a major emphasis on the mechanism of action of novel drugs under development, innovative pharmacological technologies, cell signaling, transduction pathway analysis, genomics, proteomics, and metabonomics applications to drug action. An additional focus will be the way in which normal biological function is illuminated by knowledge of the action of drugs at the cellular and molecular level. The journal publishes full-length/mini reviews, original research articles and thematic issues on molecular pharmacology. Current Molecular Pharmacology is an essential journal for every scientist who is involved in drug design and discovery, target identification, target validation, preclinical and clinical development of drugs therapeutically useful in human disease.
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