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心源性休克中心律失常的管理:米力农和多巴酚丁胺治疗的见解

Managing Arrhythmias in Cardiogenic Shock: Insights Into Milrinone and Dobutamine Therapy.

作者信息

Fletcher Jodi-Ann A, Poornima Halaharvi Savitri, Manuvel Cinda, Brooks Alexander L, Wannakuwatte Randev A, Lucano Gomez Eugenio, Ann Reid Stacy, Karnan Nithin, Reddy Snehitha, Maini Shriya, Said Bhargav A, Nazir Zahra

机构信息

Internal Medicine, St. George's University School of Medicine, St. George, GRD.

Internal Medicine, Rajiv Gandhi University of Health Sciences, Bengaluru, IND.

出版信息

Cureus. 2024 Dec 20;16(12):e76089. doi: 10.7759/cureus.76089. eCollection 2024 Dec.

Abstract

Shock is a state of inadequate perfusion that affects vital organs. Cardiogenic shock (CS) predisposes patients to various arrhythmias. The adverse effect depends on intervention and pharmacogenomics. This narrative review sheds light on treatment strategies for arrhythmias caused by milrinone and dobutamine when managing CS. Dobutamine, through beta-1 agonism, and milrinone, by phosphodiesterase-3 inhibition, increase cardiac contractility by enhancing the availability of calcium to the myocardium. Dobutamine is also a beta-2 agonist, and milrinone is a phosphodiesterase-3 inhibitor; both result in peripheral vasodilation, leading to their use preferentially in patients with CS with normotensive blood pressure. To narrow down relevant literature, various electronic databases, including PubMed, Google Scholar, and Cochrane Library, were searched. The review revealed limited evidence favoring either milrinone or dobutamine as the preferred inotropic agent for managing CS, but it did reveal that though hospital stays using dobutamine were shorter, mortality from its induced arrhythmias led to an increase in all-cause mortality rates. Both proarrhythmic agents triggered ventricular and supraventricular tachyarrhythmias, some requiring cardioversion while others are non-sustained and managed medically or symptomatically. Though neither agent has a specific reversal agent, the effect of dobutamine was seen to be successfully aborted using intravenous ultrashort half-life beta-blockers (such as esmolol). The findings accentuated the critical need for a tailored approach to managing these iatrogenic arrhythmias, emphasizing clinical vigilance and individualized patient care.

摘要

休克是一种影响重要器官的灌注不足状态。心源性休克(CS)使患者易发生各种心律失常。其不良影响取决于干预措施和药物基因组学。这篇叙述性综述阐明了在处理CS时米力农和多巴酚丁胺所致心律失常的治疗策略。多巴酚丁胺通过激动β-1受体,米力农通过抑制磷酸二酯酶-3,通过增加心肌钙的可用性来增强心脏收缩力。多巴酚丁胺也是一种β-2激动剂,米力农是一种磷酸二酯酶-3抑制剂;两者均可导致外周血管扩张,因此优先用于血压正常的CS患者。为了缩小相关文献范围,检索了包括PubMed、谷歌学术和考克兰图书馆在内的各种电子数据库。该综述显示,支持米力农或多巴酚丁胺作为处理CS首选正性肌力药物的证据有限,但确实显示,尽管使用多巴酚丁胺的住院时间较短,但其所致心律失常导致的死亡率使全因死亡率增加。两种促心律失常药物均引发室性和室上性快速心律失常,一些需要进行心脏复律,而另一些则是非持续性的,通过药物治疗或对症处理。尽管两种药物都没有特定的逆转剂,但使用静脉注射超短效β受体阻滞剂(如艾司洛尔)可成功消除多巴酚丁胺的作用。这些发现突出了对这些医源性心律失常进行个体化处理的迫切需求,强调了临床警惕性和个体化患者护理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f06f/11743927/c758284bac07/cureus-0016-00000076089-i01.jpg

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