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在感染 HIV-1 的患者中同时给予替诺福韦酯和地达诺新时细胞内核苷酸水平。

Intracellular nucleotide levels during coadministration of tenofovir disoproxil fumarate and didanosine in HIV-1-infected patients.

机构信息

Southwest CARE Center, Santa Fe, New Mexico, USA.

出版信息

Antimicrob Agents Chemother. 2011 Apr;55(4):1549-55. doi: 10.1128/AAC.00910-10. Epub 2011 Jan 31.

Abstract

Studies were conducted to determine if there is a mechanistic basis for reports of suboptimal virologic responses and concerns regarding the safety of regimens containing the combination of tenofovir (TFV) disoproxil fumarate (TDF) and didanosine (ddI) by assessing the pharmacokinetic consequences of coadministration of these drugs on intracellular nucleotides. This was a prospective and longitudinal study in HIV-1-infected patients of adding either TDF or ddI to a stable antiretroviral regimen containing the other drug. Intracellular concentrations of the nucleotide analogs TFV diphosphate (TFV-DP) and ddATP and the endogenous purine nucleotides dATP and 2'-dGTP in peripheral blood mononuclear cells were measured. A total of 16 patients were enrolled into the two study arms and a study extension. Intracellular TFV-DP concentrations (median, 120 fmol/10(6) cells) and ddATP concentrations (range, 1.50 to 7.54 fmol/10(6) cells in two patients) were unaffected following addition of ddI or TDF to a stable regimen containing the other drug. While coadministration of ddI and TDF for 4 weeks did not appear to impact dATP or dGTP concentrations, cross-sectional analysis suggested that extended therapy with ddI-containing regimens, irrespective of TDF coadministration, may decrease dATP and ddATP concentrations. Addition of TDF or ddI to a stable regimen including the other drug, in the context of ddI dose reduction, did not adversely affect the concentration of dATP, dGTP, TFV-DP, or ddATP. The association between longer-term ddI therapy and reduced intracellular nucleotide concentrations and this observation's implication for the efficacy and toxicity of ddI-containing regimens deserve further study.

摘要

研究旨在确定是否存在机制基础来解释报告中关于替诺福韦(TFV)二异丙氧膦富马酸盐(TDF)和地达诺辛(ddI)联合治疗方案中病毒学应答不理想和安全性担忧的现象,并评估这些药物联合用药对细胞内核苷酸的药代动力学影响。该研究为前瞻性、纵向研究,纳入了 HIV-1 感染患者,评估在包含其他药物的稳定抗逆转录病毒治疗方案中添加 TDF 或 ddI 的效果。外周血单个核细胞内核苷类似物 TFV 二磷酸(TFV-DP)和 ddATP 以及内源性嘌呤核苷酸 dATP 和 2'-dGTP 的浓度。共纳入 16 名患者,分为两个研究组和一个研究扩展组。在添加 ddI 或 TDF 至包含另一种药物的稳定方案中,细胞内 TFV-DP 浓度(中位数,120fmol/10(6)细胞)和 ddATP 浓度(两名患者范围为 1.50 至 7.54fmol/10(6)细胞)不受影响。虽然 ddI 和 TDF 联合用药 4 周似乎不会影响 dATP 或 dGTP 浓度,但横断面分析表明,ddI 方案的长期治疗,无论是否联合 TDF,可能会降低 dATP 和 ddATP 浓度。在减少 ddI 剂量的情况下,在包含另一种药物的稳定方案中添加 TDF 或 ddI,不会对 dATP、dGTP、TFV-DP 或 ddATP 的浓度产生不利影响。ddI 治疗时间延长与细胞内核苷酸浓度降低之间的关系及其对包含 ddI 方案的疗效和毒性的影响值得进一步研究。

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