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血清β2-微球蛋白水平在HIV感染中升高:与血清转化、CD4 T细胞减少及预后的关系。

Serum beta 2-microglobulin level increases in HIV infection: relation to seroconversion, CD4 T-cell fall and prognosis.

作者信息

Hofmann B, Wang Y X, Cumberland W G, Detels R, Bozorgmehri M, Fahey J L

机构信息

Center for Interdisciplinary Research in Immunology and Disease, UCLA (CIRID), School of Medicine 90024-1747.

出版信息

AIDS. 1990 Mar;4(3):207-14.

PMID:1972020
Abstract

Beta 2-microglobulin (beta 2-M), a marker that is increased in serum during immune activation, was investigated during the course of HIV infection. beta 2-M rose promptly in the first phase of HIV infection in people who were participating in a longitudinal study where serum samples and lymphocyte subset data were obtained at 6-monthly intervals. A rise in beta 2-M level in the first seropositive sample was seen in 93% of 50 HIV seroconverters, and those with high (or low) levels of beta 2-M at the end of year 1 tend to remain high (or low) in the ensuing years. Eighty-three per cent of seroconverters experienced a fall in CD4 T cells in the first year. The magnitude of the CD4 T-cell decline, however, did not correlate with the rise in beta 2-M in specific individuals in the first year. Nevertheless, 2-3 years after seroconversion, the initially increased beta 2-M levels did correlate inversely with the (reduced) level of CD4 T cells (P less than 0.001). Thus, the pattern of disease reflected by beta 2-M level is established in the first year of infection and persists through the following 2 years. beta 2-M levels were found to correlate with rate of CD4 T-cell fall in individuals with established HIV infection. Three groups of HIV-seropositive people with similar CD4 T-cell numbers at the first measurements (about 600-800 x 10(6)/l) but different rates of CD4 T-cell fall over the following 2 years were evaluated by beta 2-M levels. The group with stable CD4 T-cell numbers showed a significantly lower level of beta 2-M than the groups with moderately or rapidly declining CD4 T-cell numbers. Increases in beta 2-M levels during the 2 years of observation were found in people exhibiting a rapid decline in CD4 T cells (about 200 cells/year). The level of beta 2-M appears to be an indicator of HIV activity and of the rate of CD4 T-cell fall.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

β2微球蛋白(β2-M)是免疫激活期间血清中升高的一种标志物,在HIV感染过程中对其进行了研究。在一项纵向研究中,每6个月采集血清样本和淋巴细胞亚群数据,结果显示,在HIV感染的第一阶段,β2-M迅速升高。在50名HIV血清转化者中,93%的人在首次血清阳性样本中β2-M水平升高,并且在第1年末β2-M水平高(或低)的人在随后几年往往保持高(或低)水平。83%的血清转化者在第一年CD4 T细胞数量下降。然而,在第一年,特定个体中CD4 T细胞下降的幅度与β2-M的升高并无关联。尽管如此,在血清转化后2至3年,最初升高的β2-M水平确实与CD4 T细胞(降低的)水平呈负相关(P小于0.001)。因此,β2-M水平所反映的疾病模式在感染的第一年就已确立,并在接下来的两年持续存在。研究发现,β2-M水平与已确诊HIV感染个体的CD4 T细胞下降速率相关。通过β2-M水平对三组首次测量时CD4 T细胞数量相似(约600 - 800×10⁶/l)但在接下来两年中CD4 T细胞下降速率不同的HIV血清阳性人群进行了评估。CD4 T细胞数量稳定的组β2-M水平明显低于CD4 T细胞数量中度或快速下降的组。在观察的两年中,CD4 T细胞快速下降(约每年200个细胞)的人β2-M水平升高。β2-M水平似乎是HIV活性以及CD4 T细胞下降速率的一个指标。(摘要截取自250词)

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