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接受三联核苷治疗方案患者中替诺福韦二磷酸酯、卡波韦三磷酸酯和拉米夫定三磷酸酯的细胞内药代动力学。

Intracellular pharmacokinetics of tenofovir diphosphate, carbovir triphosphate, and lamivudine triphosphate in patients receiving triple-nucleoside regimens.

作者信息

Hawkins Trevor, Veikley Wenoah, St Claire Robert L, Guyer Bill, Clark Nicole, Kearney Brian P

机构信息

Southwest CARE Center, Santa Fe, NM 87505, USA.

出版信息

J Acquir Immune Defic Syndr. 2005 Aug 1;39(4):406-11. doi: 10.1097/01.qai.0000167155.44980.e8.

DOI:10.1097/01.qai.0000167155.44980.e8
PMID:16010161
Abstract

OBJECTIVE

To evaluate the potential for a pharmacologic mechanism to explain suboptimal virologic responses observed in a triple-nucleoside only regimen containing tenofovir disoproxil fumarate (TDF), abacavir (ABC), and lamivudine (3TC).

METHODS

This was a prospective evaluation of intracellular concentrations and pharmacokinetics of tenofovir diphosphate (TFV-DP), carbovir triphosphate (CBV-TP), and lamivudine triphosphate (3TC-TP) in patients on triple-nucleoside regimens. Fifteen patients on a stable TDF plus ABC plus a third nucleoside reverse transcriptase (RT) inhibitor (3TC [n = 13], stavudine [n = 2]) regimen discontinued TDF or ABC, replacing it with a nonnucleoside RT inhibitor or protease inhibitor. Peripheral blood mononuclear cells were collected after the last dose of TDF or ABC at baseline and over 12 to 96 hours as well as at days 14 and 28 after discontinuation. Nucleotide concentrations were measured directly using liquid chromatography with tandem mass spectrometry; changes after ABC or TDF discontinuation would provide evidence of an intracellular drug interaction.

RESULTS

Intracellular nucleotide concentrations of the continued drugs were unaffected when TDF or ABC was discontinued. Intracellular levels of TFV-DP exhibited less inter- and intrapatient variability than CBV-TP or 3TC-TP. TFV-DP also had persistent intracellular levels on TDF discontinuation (median half-life of 150 hours, range: 60 to >175 hours). CBV-TP concentrations fell to below the limit of detection in all patients by 72 hours after the last ABC dose in accordance with a median half-life of 18 hours (range: 12-19 hours).

CONCLUSIONS

An intracellular drug interaction does not explain the suboptimal viral response in patients treated with the nucleoside-only regimen of TDF, ABC, and 3TC.

摘要

目的

评估一种药理学机制解释在仅含替诺福韦酯富马酸盐(TDF)、阿巴卡韦(ABC)和拉米夫定(3TC)的三联核苷方案中观察到的次优病毒学反应的可能性。

方法

这是一项对接受三联核苷方案治疗的患者中替诺福韦二磷酸酯(TFV-DP)、卡波韦三磷酸酯(CBV-TP)和拉米夫定三磷酸酯(3TC-TP)的细胞内浓度和药代动力学的前瞻性评估。15名接受稳定的TDF加ABC加第三种核苷类逆转录酶(RT)抑制剂(3TC [n = 13],司他夫定 [n = 2])方案治疗的患者停用TDF或ABC,并用非核苷类RT抑制剂或蛋白酶抑制剂替代。在基线时最后一剂TDF或ABC后12至96小时以及停药后第14天和第28天收集外周血单个核细胞。使用液相色谱-串联质谱法直接测量核苷酸浓度;ABC或TDF停药后的变化将提供细胞内药物相互作用的证据。

结果

当停用TDF或ABC时,持续用药的细胞内核苷酸浓度未受影响。TFV-DP的细胞内水平在患者间和患者内的变异性小于CBV-TP或3TC-TP。TDF停药后TFV-DP的细胞内水平也持续存在(中位半衰期为150小时,范围:60至>175小时)。末次ABC剂量后72小时,所有患者的CBV-TP浓度均降至检测限以下,中位半衰期为18小时(范围:12 - 19小时)。

结论

细胞内药物相互作用不能解释接受TDF、ABC和3TC仅核苷方案治疗的患者中次优的病毒反应。

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