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首页> 外文期刊>Journal of Clinical Microbiology >Lack of Longitudinal Intrapatient Correlation between p24 Antigenemia and Levels of Human Immunodeficiency Virus (HIV) Type 1 RNA in Patients with Chronic HIV Infection during Structured Treatment Interruptions
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Lack of Longitudinal Intrapatient Correlation between p24 Antigenemia and Levels of Human Immunodeficiency Virus (HIV) Type 1 RNA in Patients with Chronic HIV Infection during Structured Treatment Interruptions

机译:结构性治疗中断期间慢性HIV感染患者中p24抗原血症与人类免疫缺陷病毒(HIV)1型RNA水平之间的纵向住院相关性缺乏

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摘要

Structured treatment interruptions (STIs) have been proposed as a potential treatment strategy during human immunodeficiency virus type 1 (HIV-1) antiretroviral therapy. This still-experimental intervention requires a close monitoring of patients' plasma viremia and CD4+-T-cell counts during the treatment interruption phase. By using signal amplification of a heat-dissociated p24 antigen (p24Ag) assay, we compared p24Ag levels with levels of HIV RNA in plasma. One hundred seventy-four plasma samples were obtained from 51 chronically HIV-infected patients: 117 from patients who underwent STIs and 57 from patients who did not. Partial immune complex dissociation and clearance of those complexes by the erythrocytes were also investigated. A significant association between the two assays was observed (β = 0.23, 95% confidence interval = 0.18, 0.28; P < 0.0001), but the association was smaller in the subset of samples from patients undergoing STIs. Moreover, discordant results and lack of longitudinal intrapatient correlation between levels of p24Ag and HIV-1 RNA were higher in this group. Incomplete immune complex dissociation and binding of those complexes to erythrocytes could be contributing factors involved in the diminished detection of p24Ag. Therefore, signal amplification of a heat-dissociated p24Ag had a positive association with current HIV RNA assays in a population-based analysis. However, it might not be sensitive enough to monitor longitudinal intrapatient viremia during STIs in patients with high CD4+-T-cell counts potentially due to the production of high-affinity anti-p24 antibodies and clearance of immune complexes by erythrocytes.
机译:已提出结构化治疗中断(STIs)作为1型人类免疫缺陷病毒(HIV-1)抗逆转录病毒治疗期间的潜在治疗策略。这种仍处于实验性的干预措施要求在治疗中断阶段密切监测患者的血浆病毒血症和CD4 + -T细胞计数。通过使用热解离的p24抗原(p24Ag)分析的信号放大,我们比较了血浆中p24Ag水平与HIV RNA水平。从51例长期感染HIV的患者中获得了174份血浆样品:其中117例进行了性传播感染的患者,57例未进行性传播感染的患者。还研究了部分免疫复合物的解离和清除这些复合物的红细胞。观察到两种测定之间的显着相关性(β= 0.23,95%置信区间= 0.18,0.28; P <0.0001),但在患有STI的患者子集中,该相关性较小。此外,该组中p24Ag和HIV-1 RNA水平之间的不一致结果和缺乏纵向的患者内部相关性更高。免疫复合物的不完全解离以及这些复合物与红细胞的结合可能是导致p24Ag检测减少的因素。因此,在基于人群的分析中,热解离的p24Ag的信号放大与当前的HIV RNA分析呈正相关。但是,对于CD4 + -T细胞计数高的患者,在性传播感染期间监测纵向患者体内病毒血症可能不够灵敏,这可能是由于产生高亲和力的抗p24抗体和清除免疫红细胞的复合物。

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