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Cytochrome P450 2B6 516G-->T is associated with plasma concentrations of nevirapine at both 200 mg twice daily and 400 mg once daily in an ethnically diverse population.细胞色素 P450 2B6 516G>T 与在一个种族多样化的人群中,每日两次 200 毫克和每日一次 400 毫克奈韦拉平的血浆浓度相关。
HIV Med. 2009 May;10(5):310-7. doi: 10.1111/j.1468-1293.2008.00689.x. Epub 2009 Feb 17.
2
Population pharmacokinetics of nevirapine in combination with rifampicin-based short course chemotherapy in HIV- and tuberculosis-infected South African patients.奈韦拉平与基于利福平的短程化疗联合应用于南非HIV和结核合并感染患者的群体药代动力学。
Eur J Clin Pharmacol. 2009 Jan;65(1):71-80. doi: 10.1007/s00228-008-0481-y. Epub 2008 Aug 27.
3
Pharmacokinetics and 48-week efficacy of nevirapine: 400 mg versus 600 mg per day in HIV-tuberculosis coinfection receiving rifampicin.奈韦拉平的药代动力学及48周疗效:在接受利福平治疗的HIV-结核合并感染患者中,每日400毫克与600毫克的对比研究
Antivir Ther. 2008;13(4):529-36.
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Nevirapine-based antiretroviral therapy started early in the course of tuberculosis treatment in adult Malawians.基于奈韦拉平的抗逆转录病毒疗法在马拉维成年患者结核病治疗过程中早期开始使用。
Antivir Ther. 2007;12(4):515-21.
5
Intracellular and plasma pharmacokinetics of nevirapine in human immunodeficiency virus-infected individuals.奈韦拉平在人类免疫缺陷病毒感染个体中的细胞内和血浆药代动力学。
Clin Pharmacol Ther. 2005 Aug;78(2):132-42. doi: 10.1016/j.clpt.2005.04.004.
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Low nevirapine plasma concentrations predict virological failure in an unselected HIV-1-infected population.在未经过挑选的HIV-1感染人群中,奈韦拉平血浆浓度低预示着病毒学治疗失败。
Clin Pharmacokinet. 2003;42(6):599-605. doi: 10.2165/00003088-200342060-00009.
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Pharmacokinetics of nevirapine: initial single-rising-dose study in humans.奈韦拉平的药代动力学:人体首次单次递增剂量研究。
Antimicrob Agents Chemother. 1993 Feb;37(2):178-82. doi: 10.1128/AAC.37.2.178.

奈韦拉平在每日服用 200 毫克或 400 毫克的情况下,在感染 HIV-1 且合并结核分枝杆菌感染的乌干达成年人中利福平的药代动力学。

Nevirapine pharmacokinetics when initiated at 200 mg or 400 mg daily in HIV-1 and tuberculosis co-infected Ugandan adults on rifampicin.

机构信息

Research Department, Infectious Diseases Institute, Makerere University College of Health Sciences, Kampala, Uganda.

出版信息

J Antimicrob Chemother. 2011 Jan;66(1):180-3. doi: 10.1093/jac/dkq411. Epub 2010 Nov 2.

DOI:10.1093/jac/dkq411
PMID:21047828
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3001850/
Abstract

BACKGROUND

rifampicin lowers nevirapine plasma concentrations by inducing cytochrome P450. However, few data are available on this interaction during the lead-in period of nevirapine treatment.

METHODS

eighteen HIV-1/tuberculosis co-infected adults receiving rifampicin daily as part of anti-tuberculosis therapy were evenly randomized to nevirapine initiation by dose escalation (NVP200) or nevirapine initiation at 200 mg twice daily (NVP400). Subjects underwent 12 h intensive pharmacokinetic sampling on Days 7, 14 and 21 of nevirapine treatment. A minimum effective concentration (MEC) of 3000 ng/mL was used to interpret nevirapine concentrations 12 h after dosing (C(12)).

TRIAL REGISTRATION NUMBER

NCT00617643 (www.clinicaltrials.gov).

RESULTS

day 7 geometric mean nevirapine C(12) [90% confidence interval (CI)] was 1504 (1127-2115) ng/mL and 3148 (2451-4687) ng/mL in the NVP200 and NVP400 arms, respectively (P < 0.01). Nevirapine C(12) on Days 14 and 21 was similar. On Day 21, nevirapine concentration in 64% of patients was below the MEC. On Day 7, geometric mean area under the curve (AUC(0-12)) was lower in the NVP200 arm, 25 223 (90% CI, 21 978-29 695) ng·h/mL versus 43 195 (35 607-57 035) ng·h/mL in the NVP400 arm (P  <  0.01). Similarly, on Day 14, nevirapine AUC(0-12) was lower in the NVP200 arm 23 668 (18 253-32 218) ng·h/mL versus the NVP400 arm 44 918 (36 264-62 769) ng·h/mL (P = 0.03).

CONCLUSIONS

in co-treated patients, nevirapine concentrations were below the MEC during initiation with dose escalation. Nevirapine initiation at the maintenance dose of 200 mg twice daily is preferred. Sub-therapeutic nevirapine concentrations were common at Day 21 with either regimen. Evaluation of higher nevirapine maintenance doses may be considered.

摘要

背景

利福平通过诱导细胞色素 P450 降低奈韦拉平的血浆浓度。然而,在奈韦拉平治疗的导入期,关于这种相互作用的资料很少。

方法

18 例 HIV-1/结核分枝杆菌合并感染的成年人在抗结核治疗中每日接受利福平治疗,随机平均分为奈韦拉平剂量递增起始组(NVP200)或奈韦拉平 200mg 每日 2 次起始组(NVP400)。在奈韦拉平治疗的第 7、14 和 21 天进行 12 小时强化药代动力学采样。使用最低有效浓度(MEC)3000ng/ml 来解释给药后 12 小时的奈韦拉平浓度(C(12))。

试验注册编号

NCT00617643(www.clinicaltrials.gov)。

结果

NVP200 组和 NVP400 组奈韦拉平 C(12)的第 7 天几何平均浓度[90%置信区间(CI)]分别为 1504(1127-2115)ng/ml 和 3148(2451-4687)ng/ml(P<0.01)。第 14 天和第 21 天的奈韦拉平 C(12)相似。第 21 天,64%的患者奈韦拉平浓度低于 MEC。第 7 天,NVP200 组奈韦拉平的曲线下面积(AUC(0-12))较低,为 25223(90%CI,21978-29695)ng·h/ml,而 NVP400 组为 43195(35607-57035)ng·h/ml(P<0.01)。同样,在第 14 天,NVP200 组奈韦拉平 AUC(0-12)为 23668(18253-32218)ng·h/ml,而 NVP400 组为 44918(36264-62769)ng·h/ml(P=0.03)。

结论

在联合治疗的患者中,奈韦拉平在剂量递增起始时的浓度低于 MEC。奈韦拉平起始维持剂量 200mg 每日 2 次更优。两种方案在第 21 天都出现了常见的奈韦拉平治疗浓度。可以考虑评估更高的奈韦拉平维持剂量。