首页> 外文期刊>Congestive heart failure. >Characterization and Prediction of Natriuretic Peptide 'Nonresponse' During Heart Failure Management: Results From the ProBNP Outpatient Tailored Chronic Heart Failure (PROTECT) and the NT-proBNP-Assisted Treatment to Lessen Serial Cardiac Readmissions and Death (BATTLESCARRED) Study
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Characterization and Prediction of Natriuretic Peptide 'Nonresponse' During Heart Failure Management: Results From the ProBNP Outpatient Tailored Chronic Heart Failure (PROTECT) and the NT-proBNP-Assisted Treatment to Lessen Serial Cardiac Readmissions and Death (BATTLESCARRED) Study

机译:心力衰竭治疗过程中利钠肽“无应答”的特征和预测:ProBNP门诊量身定制的慢性心力衰竭(PROTECT)和NT-proBNP辅助治疗可减少连续性心脏再入院和死亡的结果(BATTLESCARRED)

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Many proven heart failure (HF) therapies decrease N-terminal pro B-type natriuretic peptide (NT-proBNP) values over time, yet some patients have an NT-proBNP >1000 pg/mL following treatment, which is associated with poor outcomes. A total of 151 patients with left ventricular systolic dysfunction were treated with aggressive HF therapy in the ProBNP Outpatient Tailored Chronic Heart Failure (PROTECT) study. Clinical characteristics and NT-proBNP were measured at each visit during 10 months. In this post hoc analysis, biomarker nonresponse was defined as an NT-proBNP >1000 pg/mL and its relationship with echocardiographic and clinical characteristics and outcomes were explored. A risk model predictive of nonresponse was derived and externally validated. A rising NT-proBNP over time was associated with increased cardiovascular event rates while a decreasing NT-proBNP was associated with better clinical outcomes (58.2% vs 27.6%, P=.001). A higher percentage of time in biomarker response was associated with lower event rates (P<.001). Importantly, responders showed improved left ventricular remodeling parameters (all P<.001), while nonresponders did not. A risk model for predicting nonresponse had a C statistic of 0.82 (P<.001) and predicted outcomes well. Using data from the NT-proBNP-Assisted Treatment to Lessen Serial Cardiac Readmissions and Death (BATTLESCARRED) cohort, the risk score was validated for its ability to predict nonresponse (C statistic 0.73, P<.001). Serial changes in NT-proBNP inform risk for adverse outcome and are associated with prognostically meaningful metrics. Prediction of future NT-proBNP nonresponse to HF therapy is possible.
机译:许多行之有效的心力衰竭(HF)治疗会随着时间的流逝降低N末端pro B型利钠肽(NT-proBNP)的值,但有些患者在治疗后NT-proBNP> 1000 pg / mL,与不良预后相关。在ProBNP门诊量身定制的慢性心力衰竭(PROTECT)研究中,总共151例左室收缩功能不全患者接受了积极的HF治疗。在10个月内的每次访视中测量其临床特征和NT-proBNP。在此事后分析中,将生物标志物无反应定义为NT-proBNP> 1000 pg / mL,并探讨了其与超声心动图,临床特征和结果的关系。推导了预测无响应的风险模型并进行了外部验证。 NT-proBNP随时间升高与心血管事件发生率升高相关,而NT-proBNP降低与临床预后较好相关(58.2%vs 27.6%,P = .001)。生物标志物应答中较高的时间百分比与较低的事件发生率相关(P <.001)。重要的是,反应者显示出改善的左心室重塑参数(所有P <.001),而无反应者则没有。预测无反应的风险模型的C统计量为0.82(P <.001),并且预测结果良好。使用来自NT-proBNP辅助治疗的数据来减少系列心脏再入院和死亡(BATTLESCARRED)队列,验证了风险评分的预测无反应能力(C统计量0.73,P <.001)。 NT-proBNP的连续变化告知不良后果的风险,并与预后有意义的指标相关联。可以预测未来NT-proBNP对HF治疗无反应。

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