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儿童围生期获得性 HIV 感染者的炎症反应协调。

Coordination of inflammatory responses in children with perinatally acquired HIV infection.

机构信息

Departments of Pediatrics, Medicine, and Pathology, University of Colorado School of Medicine, Aurora, Colorado.

Centre for Biostatistics in AIDS Research, Harvard T.H. Chan School of Public Health, Boston, Massachusetts.

出版信息

AIDS. 2022 Jul 1;36(8):1117-1127. doi: 10.1097/QAD.0000000000003229. Epub 2022 Apr 19.

Abstract

OBJECTIVE

We investigated dynamics of inflammatory biomarkers in children with perinatally acquired HIV (PHIV) who started antiretrovirals at age less than 3 years and achieved sustained virologic control (HIV plasma RNA <400 copies/ml).

DESIGN

This was a retrospective analysis of inflammatory biomarkers in children enrolled in a randomized trial of early (<3 years of age) PI-based versus NNRTI-based regimens (P1060), who achieved sustained virologic control and participated in a neurodevelopmental follow-up study (P1104s) between ages 5 and 11 years.

METHODS

We measured 20 inflammatory biomarkers using ELISA or chemiluminescence at onset of sustained virologic control (Tc) and at P1104s entry (Te).

RESULTS

The 213 participants had median ages of 1.2, 1.9, and 7 years at antiretroviral initiation, Tc, and Te, respectively, with 138 on protease inhibitor-based and 74 on NNRTI-based regimens at Tc. Eighteen markers decreased and two increased from Tc to Te (Te-Tc). Biomarker subsets, particularly cytokines, the chemokine IP-10, and adhesion molecules sICAM-1 and sVCAM-1, correlated at Tc, Te, and Te-Tc. At Tc, higher biomarker levels were associated with younger age, female sex, HIV plasma RNA at least 750 000 copies/ml, lower nadir CD4 + %, lower nadir weight z scores, and NNRTI-based treatment. Greater Te-Tc biomarker declines were associated with younger age, male sex, higher Tc biomarker levels, lower nadir CD4 + %, and NNRTI-based treatment. Duration of controlled viremia and nadir height z scores showed mixed associations.

CONCLUSION

Biomarker expression showed substantial coordination. Most markers decreased after virologic control. Demographic and clinical variables associated with biomarker patterns were identified. Mechanistic studies of these biomarker patterns are needed to inform interventions to control inflammation.

摘要

目的

我们研究了在小于 3 岁时开始接受抗逆转录病毒治疗并实现持续病毒学控制(HIV 血浆 RNA<400 拷贝/ml)的围生期获得性 HIV(PHIV)儿童中,炎症生物标志物的动态变化。

设计

这是一项回顾性分析,研究对象为参加早期(<3 岁)基于蛋白酶抑制剂(PI)与基于非核苷类逆转录酶抑制剂(NNRTI)方案的随机试验(P1060)的儿童,他们实现了持续病毒学控制,并在 5 至 11 岁时参加了神经发育随访研究(P1104s)。

方法

我们使用酶联免疫吸附法或化学发光法测量了 20 种炎症生物标志物,在达到持续病毒学控制(Tc)时和进入 P1104s 时(Te)进行测量。

结果

213 名参与者的年龄中位数分别为抗逆转录病毒治疗开始时 1.2 岁、Tc 时 1.9 岁和 Te 时 7 岁,Tc 时分别有 138 名参与者接受了基于蛋白酶抑制剂的治疗,74 名参与者接受了基于 NNRTI 的治疗。有 18 种标志物从 Tc 到 Te(Te-Tc)下降,有 2 种标志物上升。生物标志物亚组,特别是细胞因子、趋化因子 IP-10、粘附分子 sICAM-1 和 sVCAM-1,在 Tc、Te 和 Te-Tc 时均具有相关性。在 Tc 时,较高的生物标志物水平与年龄较小、女性、HIV 血浆 RNA 至少为 750000 拷贝/ml、最低 CD4+%较低、最低体重 z 评分较低以及接受 NNRTI 治疗有关。更大的 Te-Tc 生物标志物下降与年龄较小、男性、更高的 Tc 生物标志物水平、更低的最低 CD4+%和接受 NNRTI 治疗有关。控制病毒血症的持续时间和最低身高 z 评分表现出混合关联。

结论

生物标志物表达表现出高度的协调性。大多数标志物在病毒学控制后下降。确定了与生物标志物模式相关的人口统计学和临床变量。需要对这些生物标志物模式进行机制研究,为控制炎症的干预措施提供信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5174/9262767/b764f6d61998/nihms-1795722-f0001.jpg

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