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环肌酸可预防缺血性损伤,并在早期再灌注期间增强心脏恢复能力。

Cyclocreatine protects against ischemic injury and enhances cardiac recovery during early reperfusion.

作者信息

Elgebaly Salwa A, Poston Robert, Todd Robert, Helmy Tarek, Almaghraby Abdallah M, Elbayoumi Tamer, Kreutzer Donald L

机构信息

Research and development, Nour Heart, Inc , Vienna , VA , USA.

Cardiothoracic Surgery, SUNY Downstate University , Brooklyn , NY , USA.

出版信息

Expert Rev Cardiovasc Ther. 2019 Sep;17(9):683-697. doi: 10.1080/14779072.2019.1662722. Epub 2019 Sep 17.

Abstract

: A critical mechanism of how hypoxia/ischemia causes irreversible myocardial injury is through the exhaustion of adenosine triphosphate (ATP). Cyclocreatine (CCr) and its water-soluble salt Cyclocreatine-Phosphate (CCrP) are potent bioenergetic agents that preserve high levels of ATP during ischemia. : CCr and CCrP treatment prior to the onset of ischemia, preserved high levels of ATP in ischemic myocardium, reduced myocardial cell injury, exerted anti-inflammatory and anti-apoptotic activities, and restored contractile function during reperfusion in animal models of acute myocardial infarction (AMI), global cardiac arrest, cardiopulmonary bypass, and heart transplantation. Medline and Embase (1970 - Feb 2019), the WIPO databank (up to Feb 2019); no language restriction. : This review provides the basis for a number of clinical applications of CCrP and CCr to minimize ischemic injury and necrosis. One strategy is to administer CCrP to AMI patients in the pre-hospital phase, as well as during, or after Percutaneous Coronary Intervention (PCI) procedure to potentially achieve protection of the myocardium, reduce infarcted-size, and, thus, limit the progression to heart failure. Another clinical applications are in predictable myocardial ischemia where pretreatment with CCrP would likely improve outcome and quality of life of patients who will undergo cardiopulmonary bypass for coronary revascularization and end-stage heart failure patients scheduled for heart transplantation.

摘要

缺氧/缺血导致不可逆心肌损伤的关键机制是三磷酸腺苷(ATP)耗竭。环肌酸(CCr)及其水溶性盐环肌酸磷酸盐(CCrP)是强效生物能量剂,可在缺血期间维持高水平的ATP。在急性心肌梗死(AMI)、心脏骤停、体外循环和心脏移植动物模型中,在缺血发作前进行CCr和CCrP治疗,可维持缺血心肌中的高水平ATP,减少心肌细胞损伤,发挥抗炎和抗凋亡活性,并在再灌注期间恢复收缩功能。检索了Medline和Embase(1970年至2019年2月)、WIPO数据库(截至2019年2月);无语言限制。本综述为CCrP和CCr的一些临床应用提供了依据,以尽量减少缺血性损伤和坏死。一种策略是在院前阶段以及经皮冠状动脉介入治疗(PCI)过程中或之后,给AMI患者使用CCrP,以潜在地实现心肌保护、减小梗死面积,从而限制向心力衰竭发展。其他临床应用是在可预测的心肌缺血中,在进行冠状动脉血运重建的体外循环患者和计划进行心脏移植的终末期心力衰竭患者中,用CCrP预处理可能会改善患者的预后和生活质量。

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