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了解体位性心动过速综合征临床试验中的安慰剂效应。

Understanding the placebo effect in clinical trials for postural tachycardia syndrome.

作者信息

Nwazue Victor C, Arnold Amy C, Raj Vidya, Black Bonnie K, Biaggioni Italo, Paranjape Sachin Y, Orozco Carlos, Dupont William D, Robertson David, Raj Satish R

机构信息

Autonomic Dysfunction Center, Division of Clinical Pharmacology, Department of Medicine, Vanderbilt University, Nashville, TN, USA.

出版信息

Clin Exp Pharmacol Physiol. 2014 May;41(5):325-30. doi: 10.1111/1440-1681.12221.

Abstract

Postural tachycardia syndrome (POTS) is characterized by excessive increases in heart rate (HR) upon standing. Previous studies have shown that standing HR decreases over time in POTS patients given placebo. We hypothesized that this reduction is due to cardiovascular physiological alteration, as opposed to psychological benefit from perceived therapy. To prospectively test this hypothesis, we examined the effects of an open-label 'no treatment' intervention (NoRx) compared with a patient-blinded placebo on standing HR in POTS patients. Twenty-one POTS patients participated in a randomized cross-over trial with oral placebo versus NoRx administered at 0900 h. Seated blood pressure (BP) and HR were measured at baseline and every hour for 4 h. Similarly, BP and HR were measured while patients stood for 10 min at these time points. Standing HR decreased significantly over time with both NoRx (112±13 and 103±16 b.p.m. at baseline and 4 h, respectively) and placebo (112±14 and 102±16 b.p.m. at baseline and 4 h, respectively; Ptime<0.001), but this effect was not different between interventions (Pdrug=0.771). Postural tachycardia syndrome patients have exaggerated orthostatic tachycardia in the morning that decreases over time with either placebo or NoRx interventions, suggesting this phenomenon is due to cardiovascular physiological variation. These data highlight the need for a placebo arm in haemodynamic clinical trials in POTS and may have important implications for the diagnosis of these patients.

摘要

体位性心动过速综合征(POTS)的特征是站立时心率(HR)过度增加。先前的研究表明,给予安慰剂的POTS患者站立时心率会随时间下降。我们假设这种下降是由于心血管生理改变,而非来自感知到的治疗的心理益处。为了前瞻性地验证这一假设,我们比较了开放标签的“无治疗”干预(NoRx)与患者盲法安慰剂对POTS患者站立心率的影响。21名POTS患者参与了一项随机交叉试验,在09:00口服安慰剂与NoRx。在基线时以及之后4小时每小时测量坐位血压(BP)和心率。同样,在这些时间点患者站立10分钟时测量血压和心率。NoRx(基线时和4小时时分别为112±13和103±16次/分钟)和安慰剂(基线时和4小时时分别为112±14和102±16次/分钟;P时间<0.001)组站立心率均随时间显著下降,但两种干预之间的这种效应无差异(P药物=0.771)。体位性心动过速综合征患者早晨的直立性心动过速更为明显,且在安慰剂或NoRx干预下均随时间下降,提示这种现象是由于心血管生理变化所致。这些数据凸显了在POTS血流动力学临床试验中设置安慰剂组的必要性,可能对这些患者的诊断具有重要意义。

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