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非洲裔与瑞士艾滋病毒队列研究中未经治疗的患者的 CD4 细胞计数下降速度较慢有关。

African descent is associated with slower CD4 cell count decline in treatment-naive patients of the Swiss HIV Cohort Study.

机构信息

Institute of Biology, Eötvös Loránd University, Budapest, Hungary.

出版信息

AIDS. 2009 Jun 19;23(10):1269-76. doi: 10.1097/QAD.0b013e32832d4096.

Abstract

OBJECTIVE

We investigated the effect of descent (African versus European) on the progression of untreated HIV infections in a prospective cohort study of HIV-1-infected individuals.

METHODS

We estimated the linear rate of decline of the CD4 cell count and the setpoint viral load in patients with sufficient data points. The effect of descent was assessed by microltivariate regression models including descent, sex, viral subtype, the earliest date of confirmed infection, age, and the baseline CD4 cell count; the rate of CD4 cell count decline was also analyzed with mixed-effect models and with matched comparisons between patients of African and European descent based on the baseline CD4 cell count.

RESULTS

We found that the decline slope of the CD4 cell count was significantly less steep (+26.6 cells/microl per year; 95% confidence interval, 12.3-41.0; P < 0.001) in patients of African descent (n = 123) compared with patients of European descent (n = 463), and this effect was independent of differences in the infecting viral subtypes. Matched comparisons confirmed the effect of African descent (P < 0.001). Remarkably, the rate of CD4 cell count decline depended strongly on the viral setpoint in patients of European descent (-46.3 cells/microl per year/log10 RNA copies/ml; 95% confidence interval, -55.8 to -36.7; P < 0.001) but not in patients of African descent.

CONCLUSION

Slower disease progression in patients of African descent might be related to host factors allowing better tolerance of high virus levels in patients of African descent compared with patients of European descent.

摘要

目的

我们通过对 HIV-1 感染者的前瞻性队列研究,调查未接受治疗的 HIV 感染者中,起源(非洲裔与欧洲裔)对疾病进展的影响。

方法

我们通过微变量回归模型,包括起源、性别、病毒亚型、首次确诊感染日期、年龄和基线 CD4 细胞计数,对有足够数据点的患者估算 CD4 细胞计数下降的线性速率和病毒载量设定点。我们还使用混合效应模型和基于基线 CD4 细胞计数的非洲裔和欧洲裔患者的匹配比较,分析 CD4 细胞计数下降率。

结果

我们发现,非洲裔患者(n = 123)的 CD4 细胞计数下降斜率明显较缓(每年增加 26.6 个细胞/微升;95%置信区间,12.3-41.0;P < 0.001),而欧洲裔患者(n = 463)则较陡,这种影响独立于感染的病毒亚型差异。匹配比较证实了非洲裔的影响(P < 0.001)。值得注意的是,在欧洲裔患者中,CD4 细胞计数下降率与病毒设定点密切相关(每年减少 46.3 个细胞/微升/对数 10 RNA 拷贝/ml;95%置信区间,-55.8 至-36.7;P < 0.001),但在非洲裔患者中则不然。

结论

非洲裔患者疾病进展较慢可能与宿主因素有关,这些因素使非洲裔患者能更好地耐受高水平的病毒,而欧洲裔患者则不能。

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