在ARROW试验中，乌干达1型艾滋病毒感染儿童每日一次与每日两次服用拉米夫定和阿巴卡韦的药代动力学及可接受性

Pharmacokinetics and acceptability of once- versus twice-daily lamivudine and abacavir in HIV type-1-infected Ugandan children in the ARROW Trial.

作者信息

Musiime Victor, Kendall Lindsay, Bakeera-Kitaka Sabrina, Snowden Wendy B, Odongo Florence, Thomason Margaret, Musoke Philippa, Adkison Kimberly, Burger David, Mugyenyi Peter, Kekitiinwa Adeodata, Gibb Diana M, Walker A Sarah

机构信息

Joint Clinical Research Centre, Kampala, Uganda.

出版信息

Antivir Ther. 2010;15(8):1115-24. doi: 10.3851/IMP1695.

DOI:10.3851/IMP1695

PMID:21149918

Abstract

BACKGROUND

No data on once-daily dosing of nucleoside analogues in African children currently exist. We compared the pharmacokinetics (PK) of once- versus twice-daily lamivudine and abacavir treatment using the World Health Organization recommended weight band dosing of scored adult tablets.

METHODS

HIV type-1 (HIV-1)-infected Ugandan children aged 3-12 years receiving antiretroviral therapy that included lamivudine and abacavir twice daily (total 150+300 mg, 225+450 mg and 225/300+600 mg daily for 12-<20, 20-<25 and ≥25 kg, respectively) were enrolled in a crossover study. Plasma PK sampling (at 0, 1, 2, 4, 6, 8 and 12 h after observed morning intake) was performed for the twice-daily regimen at steady-state. Children were then switched to once-daily treatment with PK sampling repeated 4 weeks later (with an additional 24 h sample). Acceptability questionnaires were completed at both time points. Daily area under the curve (AUC(0-24)) and maximum concentrations (C(max)) were compared by geometric mean ratios (GMRs).

RESULTS

A total of 41 HIV-1-infected children (median age of 7 years) and n=23, n=14 and n=4 in 12-<20, 20-<25 and ≥25 kg weight bands, respectively, were enrolled. Mean AUC(0-24) was 13.0 and 12.0 mg•h/l for once- and twice-daily lamivudine (GMR 1.09, 90% confidence intervals [CI] 0.98-1.20) and 15.3 and 15.6 mg•h/l for once- and twice-daily abacavir (GMR 0.98, 90% CI 0.89-1.08), respectively, with no difference in 3-6 versus 7-12 year olds. C(max) was 76% (lamivudine) and 64% (abacavir) higher on once-daily regimens. For both children and caregivers, once-daily dosing of lamivudine plus abacavir was highly acceptable and strongly preferred over twice-daily.

CONCLUSIONS

In children aged 3-12 years, AUC(0-24) of lamivudine and abacavir were bioequivalent on once- and twice-daily regimens. Once-daily dosing of abacavir and lamivudine could provide an alternative dosing strategy for HIV-1-infected children, with high acceptability and strong preference suggesting the potential for improved adherence.

摘要

背景

目前尚无关于非洲儿童每日一次服用核苷类似物的数据。我们使用世界卫生组织推荐的按体重范围给药的刻痕成人片剂，比较了每日一次与每日两次服用拉米夫定和阿巴卡韦的药代动力学（PK）。

方法

对年龄在3至12岁、接受包括拉米夫定和阿巴卡韦在内的抗逆转录病毒疗法（分别为12 - <20、20 - <25和≥25 kg体重范围的儿童，每日剂量分别为150 + 300 mg、225 + 450 mg和225/300 + 600 mg，每日两次）的乌干达HIV - 1感染儿童进行了一项交叉研究。在稳态下，对每日两次给药方案进行血浆PK采样（在观察到的早晨服药后0、1、2、4、6、8和12小时）。然后儿童改用每日一次治疗，4周后重复PK采样（额外增加一个24小时样本）。在两个时间点均完成了可接受性问卷。通过几何平均比值（GMRs）比较每日曲线下面积（AUC(0 - 24)）和最大浓度（C(max)）。

结果

共纳入41名HIV - 1感染儿童（中位年龄7岁），体重范围在12 - <20、20 - <25和≥25 kg的分别有n = 23、n = 14和n = 4。拉米夫定每日一次和每日两次给药的平均AUC(0 - 24)分别为13.0和12.0 mg•h/l（GMR 1.09，90%置信区间[CI] 0.98 - 1.20），阿巴卡韦每日一次和每日两次给药的分别为15.3和15.6 mg•h/l（GMR 0.98，90% CI 0.89 - 1.08），3 - 6岁儿童与7 - 12岁儿童之间无差异。每日一次给药方案的C(max)高76%（拉米夫定）和64%（阿巴卡韦）。对于儿童和照顾者而言，拉米夫定加阿巴卡韦每日一次给药非常可接受，且强烈优于每日两次给药。