AIDS. 1994 Jul;8(7):923-33.
To investigate the usefulness of single determinations of serum immunoglobulin (Ig) A and beta 2-microglobulin (beta 2M) levels in estimating the time from HIV seroconversion.
Five cohorts were represented in the workshop. The Multicohort Analysis Project (MAP) workshop database comprised 1744 HIV-infected patients with documented HIV seroconversion times, 363 of whom had AIDS. Overall, 1430 patients had two or more pre-AIDS CD4+ cell counts (13056 counts); 896 patients had two or more pre-AIDS IgA measurements (6081 observations); but only 2964 beta 2M measurements were available.
Marker paths for loge IgA and loge beta 2M and for square root of CD4+ cell count. Dependence on cofactors (age, sex, mode of HIV transmission) and attention to inter-individual variation in seroconversion level and annual decline in square root of CD4+ cell count. Logistic discrimination was performed using cofactor-adjusted paired loge IgA and loge beta 2M to date HIV infections as recent (within 3 years of seroconversion), intermediate, or distant (> or = 6 years after seroconversion). Transition intensities between immunologically defined states (using IgA or beta 2M) and to clinical AIDS.
Linear functional form described the decline in square root of CD4+ cell count, except for the Italian cohort where a steeper annual loss of square root of CD4+ cell count occurred in the first year than thereafter. Square root of CD4+ cell count at seroconversion depended on age and mode of transmission. Annual loss of square root of CD4+ cell count was less severe in those infected by sexual transmission. Non-monotone functional form emerged for loge IgA with an initial decrease in the first year after seroconversion followed by an increase thereafter. Loge IgA levels were higher in older subjects and in those infected by sexual transmission, but lower in women. A quadratic growth curve described the marker path for loge beta 2M, which increased for 5-6 years after seroconversion but declined thereafter. Loge beta 2M values were significantly higher in older patients and injecting drug users, but lower in women. The considerable heterogeneity of marker paths between individuals affected all three markers, but marker values appeared to track within an individual. Discrimination based on paired IgA and beta 2M measurements from single blood samples performed poorly in classifying HIV infections as recent, intermediate or distant. High intensities of backward as well as forward transitions between immunologically defined states explained the poor discrimination based on single sample per individual.
Further study of how serum IgA reflects HIV infection and careful clinical and statistical assessment of reduced beta 2M from 5 or 6 years after HIV infection are needed. The dependence of marker paths on mode of HIV transmission suggests that sexual transmission may have implications for HIV disease progression. The feasibility of using serum IgA and beta 2M, evaluable in single stored blood samples, to estimate time of HIV infection has been set back by our results.
研究单次测定血清免疫球蛋白(Ig)A和β2-微球蛋白(β2M)水平在估计HIV血清转化时间方面的作用。
研讨会上有五个队列。多队列分析项目(MAP)研讨会数据库包含1744例有记录的HIV血清转化时间的HIV感染患者,其中363例患有艾滋病。总体而言,1430例患者有两次或更多次艾滋病前CD4 +细胞计数(13056次计数);896例患者有两次或更多次艾滋病前IgA测量值(6081次观察);但仅有2964次β2M测量值。
loge IgA和loge β2M以及CD4 +细胞计数平方根的标志物轨迹。对辅助因素(年龄、性别、HIV传播方式)的依赖性以及对血清转化水平的个体间差异和CD4 +细胞计数平方根的年下降率的关注。使用经辅助因素调整的配对loge IgA和loge β2M进行逻辑判别,以确定HIV感染是近期(血清转化后3年内)、中期还是远期(血清转化后≥6年)。免疫定义状态之间(使用IgA或β2M)以及向临床艾滋病的转变强度。
线性函数形式描述了CD4 +细胞计数平方根的下降情况,但意大利队列除外,该队列中CD4 +细胞计数平方根在第一年的年损失比之后更陡峭。血清转化时CD4 +细胞计数平方根取决于年龄和传播方式。性传播感染患者的CD4 +细胞计数平方根的年损失较轻。loge IgA呈现非单调函数形式,血清转化后第一年最初下降,此后上升。老年受试者和性传播感染患者的loge IgA水平较高,但女性较低。二次增长曲线描述了loge β2M的标志物轨迹,其在血清转化后5 - 6年上升,但此后下降。老年患者和注射吸毒者的loge β2M值显著较高,但女性较低。个体间标志物轨迹的显著异质性影响了所有三个标志物,但标志物值在个体内似乎具有跟踪性。基于单次血样的配对IgA和β2M测量进行的判别在将HIV感染分类为近期、中期或远期方面表现不佳。免疫定义状态之间向前和向后的高转变强度解释了基于个体单一样本的判别不佳的原因。
需要进一步研究血清IgA如何反映HIV感染,并对HIV感染5或6年后β2M降低进行仔细的临床和统计学评估。标志物轨迹对HIV传播方式的依赖性表明性传播可能对HIV疾病进展有影响。我们的结果表明,使用单次储存血样中可评估的血清IgA和β2M来估计HIV感染时间的可行性受到了挫折。
