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维生素 K 拮抗剂与治疗范围内的时间:影响、挑战和改善策略。

Vitamin K antagonists and time in the therapeutic range: implications, challenges, and strategies for improvement.

机构信息

Department of Medicine, Boston University Medical Center, Boston, MA 02118, USA.

出版信息

J Thromb Thrombolysis. 2013 Apr;35(3):333-5. doi: 10.1007/s11239-013-0900-5.

Abstract

Oral vitamin K antagonists are highly efficacious in the prevention and treatment of thromboembolic disease. Optimal use of these agents in clinical practice is challenged by their narrow therapeutic window. The proportion of time spent in the International Normalized Ratio (INR) range of 2.0-3.0 [time in the therapeutic range (TTR)] has been closely associated with adverse outcomes, i.e., stroke, hemorrhage, mortality. Although TTR is a validated marker, it has several limitations. TTR does not capture short-term risks associated with highly variable periods or periods characterized by extreme deviations in INR. Because TTR measurement is limited to consecutive periods of warfarin exposure, it does not inform the risks associated with gap periods of 56 days or greater as these time intervals are excluded from end-point rate calculations. Because individuals with gaps in monitoring represent a different patient population than those without gaps, e.g., less adherent, more acutely ill, more frequent transitions in health status, TTR analyses are likely most valid and informative for individuals with uninterrupted monitoring of the INR. Duration of warfarin therapy and patient-specific factors have also been shown to influence TTR. Younger age, female sex, lower income, black race, frequent hospitalizations, polypharmacy, active cancer, decompensated heart failure, substance abuse, psychiatric disorders, dementia, and chronic liver disease have all been associated with lower TTR. Targeted strategies to improve TTR are urgently needed.

摘要

口服维生素 K 拮抗剂在预防和治疗血栓栓塞性疾病方面非常有效。在临床实践中,这些药物的最佳使用受到其狭窄治疗窗口的挑战。国际标准化比值 (INR) 范围内的时间比例(即治疗范围内的时间 (TTR))与不良结局(即中风、出血、死亡率)密切相关。尽管 TTR 是一个经过验证的标志物,但它有几个局限性。TTR 不能捕捉与 INR 高度变化期或极端偏差期相关的短期风险。由于 TTR 测量仅限于华法林暴露的连续期间,因此它不会告知与 56 天或更长时间的间隙期相关的风险,因为这些时间间隔被排除在终点率计算之外。由于监测间隙期的个体代表了与没有间隙期的个体不同的患者群体,例如,不那么依从、病情更急性、健康状况更频繁转变,因此 TTR 分析可能对 INR 监测不间断的个体最有效和最有信息。华法林治疗的持续时间和患者特定因素也已被证明会影响 TTR。年龄较小、女性、收入较低、黑种人、频繁住院、多种药物治疗、活动性癌症、失代偿性心力衰竭、药物滥用、精神障碍、痴呆症和慢性肝脏疾病均与 TTR 降低有关。迫切需要针对提高 TTR 的策略。

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