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首页> 外文期刊>The Journal of Infectious Diseases >Evaluation of human immunodeficiency virus (HIV) type 1 load, CD4 T cell level, and clinical class as time-fixed and time-varying markers of disease progression in HIV-1-infected children.
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Evaluation of human immunodeficiency virus (HIV) type 1 load, CD4 T cell level, and clinical class as time-fixed and time-varying markers of disease progression in HIV-1-infected children.

机译:评价人类免疫缺陷病毒(HIV)1型负荷,CD4 T细胞水平和临床类别作为感染HIV-1的儿童疾病进展的时标和时变标志。

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摘要

Human immunodeficiency virus (HIV) type 1 RNA load, CD4 T cell level, and Centers for Disease Control and Prevention (CDC) clinical class history were measured as potential correlates of a CDC class C diagnosis or death in 165 HIV-1-infected children followed from birth. These covariates were assessed at fixed "landmark" ages from 6 to 24 months and were also assessed as time-varying values. Virus load was associated with progression in all analyses, even after adjusting for immunologic and clinical status. This confirms its importance for monitoring pediatric disease progression. CD4 T cell level was associated with disease progression in time-varying but not in adjusted landmark analysis, suggesting that CD4 cells reflects immediate risk more than long-term risk. The distinction between clinical class B and lower classes is prognostic during the first 18 months of life; class C versus classes N/A/B becomes more important as the patient ages. Virologic, immunologic, and clinical status all provide information regarding disease progression risk.
机译:测量了人类免疫缺陷病毒(HIV)1型RNA载量,CD4 T细胞水平以及疾病控制与预防中心(CDC)临床分类史,作为165名感染HIV-1的儿童CDC C类诊断或死亡的潜在相关因素从出生开始。这些协变量是在固定的“具有里程碑意义的”年龄6到24个月时评估的,也被视为随时间变化的值。即使调整了免疫学和临床状况,所有分析中的病毒载量也与进展相关。这证实了其对于监测儿科疾病进展的重要性。 CD4 T细胞水平随时间变化与疾病进展相关,但在调整后的地标分析中却不相关,这表明CD4细胞反映的直接风险大于长期风险。临床B级和低级之间的区别是在生命的头18个月内是预后的;随着患者年龄的增长,C级对N / A / B级变得越来越重要。病毒学,免疫学和临床状态均提供有关疾病进展风险的信息。

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