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Metabolic Rates of ATP Transfer Through Creatine Kinase (CK Flux) Predict Clinical Heart Failure Events and Death

机译:ATP通过肌酸激酶(CK Flux)转移的代谢率可预测临床心力衰竭事件和死亡

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Morbidity and mortality from heart failure (HF) are high, and current risk stratification approaches for predicting HF progression are imperfect. Adenosine triphosphate (ATP) is required for normal cardiac contraction, and abnormalities in creatine kinase (CK) energy metabolism, the primary myocardial energy reserve reaction, have been observed in experimental and clinical HF. However, the prognostic value of abnormalities in ATP production rates through CK in human HF has not been investigated. Fifty-eight HF patients with nonischemic cardiomyopathy underwent P-31 magnetic resonance spectroscopy (MRS) to quantify cardiac high-energy phosphates and the rate of ATP synthesis through CK (CK flux) and were prospectively followed for a median of 4.7 years. Multiple-event analysis (MEA) was performed for HF-related events including all-cause and cardiac death, HF hospitalization, cardiac transplantation, and ventricular-assist device placement. Among baseline demographic, clinical, and metabolic parameters, MEA identified four independent predictors of HF events: New York Heart Association (NYHA) class, left ventricular ejection fraction (LVEF), African-American race, and CK flux. Reduced myocardial CK flux was a significant predictor of HF outcomes, even after correction for NYHA class, LVEF, and race. For each increase in CK flux of 1 mu mol g(-1) s(-1), risk of HF-related composite outcomes decreased by 32 to 39%. These findings suggest that reduced CK flux may be a potential HF treatment target. Newer imaging strategies, including noninvasive P-31 MRS that detect altered ATP kinetics, could thus complement risk stratification in HF and add value in conditions involving other tissues with high energy demands, including skeletal muscle and brain.
机译:心力衰竭(HF)的发病率和死亡率很高,目前用于预测HF进展的风险分层方法并不完善。正常的心脏收缩需要三磷酸腺苷(ATP),并且在实验和临床HF中已观察到肌酸激酶(CK)能量代谢异常(主要的心肌能量储备反应)异常。然而,尚未研究通过CK在人HF中ATP产生速率异常的预后价值。 58例非缺血性心肌病的HF患者接受了P-31磁共振波谱(MRS)量化心脏高能磷酸盐和通过CK的ATP合成速率(CK通量),预期随访时间中位数为4.7年。对HF相关事件进行了多事件分析(MEA),包括全因和心脏死亡,HF住院,心脏移植和心室辅助器械放置。在基线人口统计学,临床和代谢参数中,MEA确定了HF事件的四个独立预测因子:纽约心脏协会(NYHA)类,左心室射血分数(LVEF),非裔美国人种族和CK通量。即使校正了NYHA等级,LVEF和种族,心肌CK通量降低也是HF预后的重要预测指标。 CK通量每增加1μmol g(-1)s(-1),与HF相关的复合结果的风险降低32%至39%。这些发现表明降低的CK通量可能是潜在的HF治疗目标。较新的成像策略,包括检测ATP动力学改变的无创P-31 MRS,可以补充心衰风险分层,并在涉及其他高能量需求组织(包括骨骼肌和大脑)的情况下增加价值。

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