血浆药物水平验证了自我报告的依从性,但预测了抗逆转录病毒治疗不依从性的有限特异性。

ISRN Pharmacology Pub Date : 2012-01-01 Epub Date: 2012-03-06 DOI:10.5402/2012/274978
Robert Balikuddembe, Joshua Kayiwa, David Musoke, Muhammad Ntale, Steven Baveewo, Paul Waako, Celestino Obua
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引用次数: 5

摘要

介绍。在低收入国家,抗逆转录病毒治疗(ART)的依从性主要通过自我报告的依从性(S-RA)来评估,而不需要测定药物水平。不依从性是出现抗逆转录病毒治疗耐药的一个重要因素,因此需要确定药物水平。目标。我们着手建立血浆司他夫定水平与S-RA之间的关系,并根据实际血浆药物浓度验证S-RA。方法。一项涉及乌干达234例患者的横断面调查。高效液相色谱法测定司他夫定血浆水平。我们使用多变量logistic回归模型比较了司他夫定和S-RA的血浆水平类别。结果。总体而言,194/234例患者S-RA≥95%(依从性好),166/234例他夫定血药浓度≥36 nmol/L(治疗浓度)。S-RA良好患者的司他夫定水平在治疗浓度范围内的可能性是正常患者的8倍(校正优势比:7.7,95%可信区间:3.5-7.0)。然而,在194例S-RA良好的患者中,21.7%的患者浓度低于治疗浓度。S-RA对依从性的敏感性高(91.6%),但对内在不良依从性的特异性有限(38.2%)。结论。S-RA是评估依从性的良好工具,但在检测不依从性方面特异性较低,这可能会导致耐药性的出现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Plasma drug level validates self-reported adherence but predicts limited specificity for nonadherence to antiretroviral therapy.

Plasma drug level validates self-reported adherence but predicts limited specificity for nonadherence to antiretroviral therapy.

Introduction. Adherence to antiretroviral therapy (ART) in low-income countries is mainly assessed by self-reported adherence (S-RA) without drug level determination. Nonadherence is an important factor in the emergence of resistance to ART, presenting a need for drug level determination. Objective. We set out to establish the relationship between plasma stavudine levels and S-RA and validate S-RA against the actual plasma drug concentrations. Methods. A cross-sectional investigation involving 234 patients in Uganda. Stavudine plasma levels were determined using high-performance liquid chromatography. We compared categories of plasma levels of stavudine with S-RA using multivariable logistic regression models. Results. Overall, 194/234 patients had S-RA ≥ 95% (good adherence) and 166/234 had stavudine plasma concentrations ≥ 36 nmol/L (therapeuticconcentration). Patients with good S-RA were eight times more likely to have stavudine levels within therapeutic concentration (Adjusted Odds Ratio: 7.7, 95% Confidence Interval: 3.5-7.0). However, of the 194 patients with good S-RA, 21.7% had below therapeutic concentrations. S-RA had high sensitivity for adherence (91.6%), but limited specificity for intrinsic poor adherence (38.2%). Conclusions. S-RA is a good tool for assessing adherence, but has low specificity in detecting nonadherence, which has implications for emergence of resistance.

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