南非抗逆转录病毒治疗期间CD4细胞恢复与结核病的短期和长期风险

Short-term and long-term risk of tuberculosis associated with CD4 cell recovery during antiretroviral therapy in South Africa.

作者信息

Lawn Stephen D, Myer Landon, Edwards David, Bekker Linda-Gail, Wood Robin

机构信息

The Desmond Tutu HIV Centre, Institute for Infectious Disease and Molecular Medicine, Faculty of Health Sciences, University of Cape Town, Cape Town, South Africa.

出版信息

AIDS. 2009 Aug 24;23(13):1717-25. doi: 10.1097/QAD.0b013e32832d3b6d.

Abstract

OBJECTIVE

To determine the short-term and long-term risks of tuberculosis (TB) associated with CD4 cell recovery during antiretroviral therapy (ART).

DESIGN

Observational community-based ART cohort in South Africa.

METHODS

TB incidence was determined among patients (n = 1480) receiving ART for up to 4.5 years in a South African community-based service. Updated CD4 cell counts were measured 4-monthly. Person-time accrued within a range of CD4 cell count strata (CD4 cell strata) was calculated and used to derive CD4 cell-stratified TB rates. Factors associated with incident TB were identified using Poisson regression models.

RESULTS

Two hundred and three cases of TB were diagnosed during 2785 person-years of observation (overall incidence, 7.3 cases/100 person-years). During person-time accrued within CD4 cell strata 0-100, 101-200, 201-300, 301-400, 401-500 and more than 500 cells/microl unadjusted TB incidence rates were 16.8, 9.3, 5.5, 4.6, 4.2 and 1.5 cases/100 person-years, respectively (P < 0.001). During early ART (first 4 months), adjusted TB rates among those with CD4 cell counts 0-200 cells/microl were 1.7-fold higher than during long-term ART (P = 0.026). Updated CD4 cell counts were the only patient characteristic independently associated with long-term TB risk.

CONCLUSION

Updated CD4 cell counts were the dominant predictor of TB risk during ART in this low-resource setting. Among those with baseline CD4 cell counts less than 200 cells/microl, the excess adjusted risk of TB during early ART was consistent with 'unmasking' of disease missed at baseline screening. TB incidence rates at CD4 cell counts of 200-500 cells/microl remained high and adjunctive interventions are required. TB prevention would be improved by ART policies that minimized the time patients spend with CD4 cell counts below a threshold of 500 cells/microl.

摘要

目的

确定抗逆转录病毒治疗(ART)期间CD4细胞恢复与结核病(TB)的短期和长期风险。

设计

南非基于社区的ART观察队列。

方法

在南非一项基于社区的服务中,对接受ART长达4.5年的患者(n = 1480)的结核病发病率进行了测定。每4个月测量一次更新的CD4细胞计数。计算在一系列CD4细胞计数分层(CD4细胞分层)范围内累积的人时,并用于得出CD4细胞分层的结核病发病率。使用泊松回归模型确定与新发结核病相关的因素。

结果

在2785人年的观察期内诊断出203例结核病(总发病率,7.3例/100人年)。在CD4细胞分层0 - 100、101 - 200、201 - 300、301 - 400、401 - 500和超过500个细胞/微升内累积的人时中,未经调整的结核病发病率分别为16.8、9.3、5.5、4.6、4.2和1.5例/100人年(P < 0.001)。在ART早期(前4个月),CD4细胞计数为0 - 200个细胞/微升的患者中,调整后的结核病发病率比长期ART期间高1.7倍(P = 0.026)。更新的CD4细胞计数是唯一与长期结核病风险独立相关的患者特征。

结论

在这种资源匮乏的环境中,更新的CD4细胞计数是ART期间结核病风险的主要预测指标。在基线CD4细胞计数低于200个细胞/微升的患者中,ART早期结核病调整后风险增加与基线筛查时漏诊疾病的“暴露”一致。CD4细胞计数为200 - 500个细胞/微升时的结核病发病率仍然很高,需要辅助干预措施。通过ART政策将患者CD4细胞计数低于500个细胞/微升阈值的时间减至最短,可改善结核病预防。

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