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首页> 外文期刊>Journal of infection and chemotherapy: official journal of the Japan Society of Chemotherapy >Urinary beta-2 microglobulin and alpha-1 microglobulin are useful screening markers for tenofovir-induced kidney tubulopathy in patients with HIV-1 infection: A diagnostic accuracy study
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Urinary beta-2 microglobulin and alpha-1 microglobulin are useful screening markers for tenofovir-induced kidney tubulopathy in patients with HIV-1 infection: A diagnostic accuracy study

机译:尿液中的β-2微球蛋白和α-1微球蛋白是替诺福韦诱导的HIV-1感染肾小管病变的有用筛选标志物:诊断准确性研究

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Kidney tubulopathy is a well-known adverse event of antiretroviral agent tenofovir. A cross-sectional study was conducted to compare the diagnostic accuracy of five tubular markers, with a collection of abnormalities in these markers as the reference standard. The study subjects were patients with HIV-1 infection on ritonavir-boosted darunavir plus tenofovir/emtricitabine with suppressed viral load. Kidney tubular dysfunction (KTD) was predefined as the presence of at least three abnormalities in the following five parameters: β2-microglobulinuria (β2M), α1-microglobulinuria (α1M), high urinary N-acetyl-β-d-glucosaminidase (NAG), fractional excretion of phosphate (FEIP), and fractional excretion of uric acid (FE UA). Receiver operating characteristic curves and areas under the curves (AUC) were estimated, and the differences between the largest AUC and each of the other AUCs were tested using a nonparametric method. The cutoff value of each tubular marker was determined using raw data of 100 % sensitivity with maximal specificity. KTD was diagnosed in 19 of the 190 (10 %) patients. The AUCs (95 % CIs) of each tubular marker were β2M, 0.970 (0.947-0.992); α1M, 0.968 (0.944-0.992); NAG, 0.901 (0.828-0.974); FEIP, 0.757 (0.607-0.907), and FEUA, 0.762 (0.653-0.872). The AUCs of β2M and α1M were not significantly different, whereas those of the other three markers were smaller. The optimal cutoff values with 100 % sensitivity were 1,123 μg/gCr (β2M, specificity 89 %), 15.4 mg/gCr (α1M, specificity 87 %), 3.58 U/gCr (NAG, specificity 46 %), 1.02 % (FEIP, specificity 0 %), and 3.92 % (FEUA, specificity 12 %). Urinary β2M and α1M are potentially suitable screening tools for tenofovir-induced KTD. Monitoring either urinary β2M or α1M should be useful in early detection of tenofovir nephrotoxicity.
机译:肾小管病变是抗逆转录病毒药物替诺福韦的众所周知的不良事件。进行了一项横断面研究,以比较五个管状标记的诊断准确性,并以这些标记的异常情况作为参考标准。研究对象是在病毒载量受抑制的利托那韦增强的达鲁那韦加替诺福韦/恩曲他滨上感染HIV-1的患者。肾小管功能障碍(KTD)预定义为在以下五个参数中至少存在三个异常:β2-微球蛋白尿(β2M),α1-微球蛋白尿(α1M),高尿N-乙酰基-β-d-氨基葡萄糖苷酶(NAG) ,磷酸盐的部分排泄物(FEIP)和尿酸的部分排泄物(FE UA)。估算接收器工作特性曲线和曲线下面积(AUC),并使用非参数方法测试最大AUC与其他每个AUC之间的差异。使用100%灵敏度和最大特异性的原始数据确定每个管状标记的临界值。 190名患者中有19名(10%)被诊断出KTD。每个肾小管标志物的AUC(95%CI)为β2M,0.970(0.947-0.992); α1M,0.968(0.944-0.992); NAG,0.901(0.828-0.974); FEIP 0.757(0.607-0.907)和FEUA 0.762(0.653-0.872)。 β2M和α1M的AUC没有显着差异,而其他三个标记的AUC较小。灵敏度为100%的最佳截止值是1,123μg/ gCr(β2M,特异性89%),15.4 mg / gCr(α1M,特异性87%),3.58 U / gCr(NAG,特异性46%),1.02%(FEIP,特异性为0%)和3.92%(FEUA,特异性为12%)。尿中β2M和α1M是替诺福韦诱导的KTD的潜在筛选工具。监测尿β2M或α1M对早期检测替诺福韦的肾毒性应是有用的。

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