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接受一线抗逆转录病毒治疗的儿童的长期病毒学结局

Long-term virological outcome in children receiving first-line antiretroviral therapy.

作者信息

Chandrasekaran Padmapriyadarsini, Shet Anita, Srinivasan Ramalingam, Sanjeeva G N, Subramanyan Sudha, Sunderesan Suba, Ramesh Karunaianantham, Gopalan Bindu, Suresh Elumalai, Poornagangadevi Navaneethan, Hanna Luke E, Chandrasekar Chockalingam, Wanke Christine, Swaminathan Soumya

机构信息

Department of Clinic Research, ICMR-National Institute for Research in Tuberculosis, No. 1, Mayor Sathyamoorthy Road, Chetpet, Chennai, Tamil Nadu, 600031, India.

Johns Hopkins Bloomberg School of Public Health, Baltimore, USA.

出版信息

AIDS Res Ther. 2018 Nov 26;15(1):23. doi: 10.1186/s12981-018-0208-9.

Abstract

BACKGROUND

Studies relating to long-term virological outcomes among children on first-line antiretroviral therapy (ART) from low and middle-income countries are limited.

METHODS

Perinatally HIV infected, ART-naive children, between 2 and 12 years of age, initiating NNRTI-based ART during 2010-2015, with at least 12 months of follow-up, were included in the analysis. CD4 cell counts and plasma HIV-1 RNA were measured every 24 weeks post-ART initiation. Immunologic failure was defined as a decrease in the CD4 count to pre-therapy levels or below and virologic failure as HIV-RNA of > 1000 copies/ml at 48 weeks after ART initiation. Genotypic resistance testing was performed for children with virologic failure. Logistic regression analysis was done to identify predictors of virologic failure.

RESULTS

Three hundred and ninety-three ART-naïve children living with HIV [mean (SD) age: 7.6 (3) years; mean (SD) CD4%: 16% (8); median (IQR) HIV-RNA: 5.1 (3.5-5.7) log copies/ml] were enrolled into the study. At 48 weeks, significant improvement occurred in weight-for-age and height-for-age z-scores from baseline (all p < 0.001). The immunologic response was good; almost 90% of children showing an increase in their absolute CD4 T cell count to more than 350 cells/mm. Immunological failure was noted among 11% (28/261) and virologic failure in 29% (94/328) of children. Of the 94 children with virologic failure at 12 months, 36 children showed immunologic failure while the rest had good immunologic improvement. There was no demonstrable correlation between virologic and immunologic failure. 62% had reported > 90% adherence to ART. At the time of virologic failure, multiple NNRTI-associated mutations were observed: 80%-K103N and Y181C being the major NNRTI mutations-observed. Sensitivity (95% CI) of immunologic failure to detect virologic failure was 7% (2-12), specificity 97% (92.4-98.9), PPV 44% (13.7-78.8) and NPV was 72% (65-77.9). There were no statistically significant predictors to detect children who will develop virologic failure on treatment.

CONCLUSIONS

Considerable immunological improvement is seen in children with ART initiation, but may not be an effective tool to monitor treatment response in the long-term. There is a lack of correlation between immunologic and virologic response while on ART, which may lead to a delay in identifying treatment failures. Periodic viral load monitoring is, therefore, a priority.

摘要

背景

关于低收入和中等收入国家接受一线抗逆转录病毒治疗(ART)的儿童长期病毒学转归的研究有限。

方法

纳入2010年至2015年期间开始基于非核苷类逆转录酶抑制剂(NNRTI)进行ART治疗、年龄在2至12岁、围产期感染HIV且未接受过ART治疗、随访至少12个月的儿童进行分析。ART治疗开始后每24周测量CD4细胞计数和血浆HIV-1 RNA水平。免疫失败定义为CD4计数降至治疗前水平或更低,病毒学失败定义为ART治疗开始后48周时HIV-RNA>1000拷贝/ml。对病毒学失败的儿童进行基因型耐药检测。采用逻辑回归分析确定病毒学失败的预测因素。

结果

393例未接受过ART治疗的HIV感染儿童[平均(标准差)年龄:7.6(3)岁;平均(标准差)CD4%:16%(8);中位数(四分位间距)HIV-RNA:5.1(3.5 - 5.7)log拷贝/ml]纳入本研究。48周时,年龄别体重和年龄别身高Z评分较基线有显著改善(所有p<0.001)。免疫反应良好;近90%的儿童绝对CD4 T细胞计数增加至超过350个细胞/mm。11%(28/261)的儿童出现免疫失败,29%(94/328)的儿童出现病毒学失败。在12个月时出现病毒学失败的94例儿童中,36例出现免疫失败,其余儿童免疫功能有良好改善。病毒学失败与免疫失败之间无明显相关性。62%的儿童报告ART依从性>90%。在病毒学失败时,观察到多个与NNRTI相关的突变:80% - K103N和Y181C为主要观察到的NNRTI突变。免疫失败检测病毒学失败的敏感性(95%CI)为7%(2 - 12),特异性为97%(92.4 - 98.9),阳性预测值为44%(13.7 - 78.8),阴性预测值为72%(65 - 77.9)。在治疗中未发现有统计学意义的预测因素来识别会发生病毒学失败的儿童。

结论

开始ART治疗的儿童免疫功能有显著改善,但可能不是长期监测治疗反应的有效工具。ART治疗期间免疫反应与病毒学反应之间缺乏相关性,这可能导致治疗失败的识别延迟。因此,定期监测病毒载量是优先事项。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9e8/6260781/f47982ce581d/12981_2018_208_Fig1_HTML.jpg

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