From the Technical Assistance and Sustainability, EGPAF, Washington, DC.
National AIDS & STI Control Program, Ministry of Health, Nairobi, Kenya.
Pediatr Infect Dis J. 2018 Jul;37(7):669-672. doi: 10.1097/INF.0000000000001843.
Data are limited on the selection and sequencing of second-line and third-line pediatric antiretroviral treatment (ART) in resource-limited settings. This study aimed to evaluate characteristics of African pediatric patients initiated on darunavir (DRV) and/or etravirine (ETR) through a specific drug donation program.
This was a cross-sectional study of baseline immunologic, virologic and demographic characteristics of children and adolescents initiating DRV-based and/or ETR-based ART. Descriptive statistics were used.
Study enrolled 48 patients (45.8% women; median age = 15 years [interquartile range 17.7-10.3]) at 9 clinical sites in Zambia, Swaziland, Kenya and Lesotho. The majority (87.5%; n = 42) had received ≥2 prior ART regimens; most (81.2%) had received lopinavir/ritonavir-based ART before switch. All patients had detectable HIV RNA (median = 56,653 copies/mL). Forty seven patients (98.9%) had HIV genotype results: 41 (87.2%) had ≥1 nucleos(t)ide reverse transcriptase inhibitor (NRTI)-resistance mutation (RM), predominantly M184V (76.6%; n = 36); 31 (65.9%) had ≥1 non-NRTI-RM, including 27 (57.4%) with ≥1 ETR-RM; 30 (63.8%) had ≥3 protease inhibitor RM, including 20 (42.6%) with ≥1 DRV-RM. For new ART regimens, DRV and raltegravir were most frequently prescribed (83.3%; n = 40 on DRV and raltegravir, each). Eighteen patients (37.5%) were initiated on the NRTI-sparing ART.
In our study, a significant proportion of treatment-experienced African children and adolescents had one or more DRV-RM and ETR-RM. For the new regimen, more than a third of pediatric patients failing second-line ART were prescribed NRTI-sparing regimens. Better understanding of the current approaches to pediatric ART sequencing in resource-limited settings is needed.
在资源有限的环境下,二线和三线儿科抗逆转录病毒治疗(ART)的选择和方案制定的数据有限。本研究旨在评估通过特定药物捐赠计划接受达芦那韦(DRV)和/或依曲韦林(ETR)治疗的非洲儿科患者的特征。
这是一项在赞比亚、斯威士兰、肯尼亚和莱索托的 9 个临床点开展的、关于开始基于 DRV 和/或 ETR 的 ART 的儿童和青少年的基线免疫、病毒学和人口统计学特征的横断面研究。使用描述性统计进行分析。
研究纳入了 48 名患者(45.8%为女性;中位年龄为 15 岁[四分位距 17.7-10.3]),他们来自赞比亚、斯威士兰、肯尼亚和莱索托的 9 个临床点。大多数(87.5%;n=42)接受过≥2 种 ART 方案;大多数(81.2%)在转换前接受过洛匹那韦/利托那韦为基础的 ART。所有患者均有可检测到的 HIV RNA(中位数=56653 拷贝/ml)。47 名患者(98.9%)有 HIV 基因型结果:41 名(87.2%)有≥1 种核苷(酸)逆转录酶抑制剂(NRTI)耐药突变(RM),主要为 M184V(76.6%;n=36);31 名(65.9%)有≥1 种非 NRTI-RM,包括 27 名(57.4%)有≥1 种 ETR-RM;30 名(63.8%)有≥3 种蛋白酶抑制剂 RM,包括 20 名(42.6%)有≥1 种 DRV-RM。新的 ART 方案中,DRV 和拉替拉韦最常被开(83.3%;n=40 名患者接受 DRV 和拉替拉韦治疗)。18 名患者(37.5%)开始使用无 NRTI 的 ART。
在我们的研究中,大量接受过治疗的非洲儿童和青少年有 1 种或多种 DRV-RM 和 ETR-RM。对于新的方案,三分之一以上二线 ART 失败的儿科患者接受了无 NRTI 的方案。需要更好地了解资源有限环境下儿科 ART 排序的当前方法。
