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使用免疫标记物和连续时间马尔可夫模型估计男同性恋者中HIV感染的进展情况。

Use of immunological markers and continuous-time Markov models to estimate progression of HIV infection in homosexual men.

作者信息

Hendriks J C, Satten G A, Longini I M, van Druten H A, Schellekens P T, Coutinho R A, van Griensven G J

机构信息

Department of Public Health, Municipal Health Service, Amsterdam, The Netherlands.

出版信息

AIDS. 1996 Jun;10(6):649-56. doi: 10.1097/00002030-199606000-00011.

Abstract

OBJECTIVES

We used continuous-time Markov models based on CD4 cell counts and anti-CD3 reactivity (i.e., measure for T-cell quality) to study the progression of HIV infection in a cohort study of homosexual men in Amsterdam. We also compared the effectiveness of anti-CD3 reactivity as a marker for disease progression with that of CD4 cell counts.

METHODS

We used data from 467 men (6905 visits) with visits at 3-month intervals between October 1984 and March 1993. To account for measurement error and short time-scale variability, the immunological stage at each visit was determined using a kernel smoother on log-transformed data from each individual. The Markov model had six marker-defined stages and a seventh stage for clinical AIDS. The initial stage-occupation probabilities for seroconverters were used to estimate the incubation time from infection to AIDS. Confidence intervals were calculated using the bootstrap method to account for the effect of smoothing on the variability of our estimates.

RESULTS

The CD4 staging scheme estimated the median time from seroconversion to AIDS at 8.3 years [95% confidence interval (CI), 8.1-8.6], and a similar estimate was obtained with the anti-CD3 staging model. The CD4 model predicts that 10.2% (95% CI, 9.9-13.1) will remain AIDS-free 15 years after seroconversion. The mean number of stages visited before AIDS is lower with the CD4 model (7.4; 95% CI, 7.2-7.7) than with the anti-CD3 model (11.3; 95% CI, 10.8-12.0), implying that anti-CD3 predicts progression less well than CD4 cell count.

CONCLUSIONS

CD4 lymphocyte counts and anti-CD3 reactivity are each associated with an increased hazard for progression to AIDS. Therefore, men in different CD4-stages (anti-CD3 stages) follow different incubation period distributions to AIDS. However, anti-CD3 predicts progression less well than CD4 cell count. Staged time-continuous Markov models are useful to study immunological markers for HIV disease progression.

摘要

目的

在阿姆斯特丹一项针对男同性恋者的队列研究中,我们使用基于CD4细胞计数和抗CD3反应性(即T细胞质量的测量指标)的连续时间马尔可夫模型来研究HIV感染的进展情况。我们还比较了抗CD3反应性作为疾病进展标志物与CD4细胞计数的有效性。

方法

我们使用了1984年10月至1993年3月期间467名男性(6905次就诊)的数据,这些男性每隔3个月就诊一次。为了考虑测量误差和短时间尺度的变异性,每次就诊时的免疫阶段通过对每个个体经对数转换的数据使用核平滑器来确定。马尔可夫模型有六个由标志物定义的阶段以及一个临床艾滋病阶段。血清转化者的初始阶段占据概率用于估计从感染到艾滋病的潜伏期。使用自助法计算置信区间,以考虑平滑对我们估计值变异性的影响。

结果

CD4分期方案估计从血清转化到艾滋病的中位时间为8.3年[95%置信区间(CI),8.1 - 8.6],抗CD3分期模型也得到了类似的估计。CD4模型预测,血清转化15年后,10.2%(95% CI,9.9 - 13.1)的人将保持无艾滋病状态。CD4模型在艾滋病出现前访问的平均阶段数(7.4;95% CI,7.2 - 7.7)低于抗CD3模型(11.3;95% CI,10.8 - 12.0),这意味着抗CD3预测进展的能力不如CD4细胞计数。

结论

CD4淋巴细胞计数和抗CD3反应性均与进展为艾滋病的风险增加相关。因此,处于不同CD4阶段(抗CD3阶段)的男性到艾滋病的潜伏期分布不同。然而,抗CD3预测进展的能力不如CD4细胞计数。分阶段的时间连续马尔可夫模型对于研究HIV疾病进展的免疫标志物很有用。

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