首页> 美国卫生研究院文献>Journal of Clinical Microbiology >MT-2 cell tropism as prognostic marker for disease progression in human immunodeficiency virus type 1 infection.
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MT-2 cell tropism as prognostic marker for disease progression in human immunodeficiency virus type 1 infection.

机译:MT-2细胞向性作为人类免疫缺陷病毒1型感染疾病进展的预后标志。

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摘要

The ability of human immunodeficiency virus type 1 (HIV-1) isolates to replicate in MT-2 cells was investigated as a prognostic marker for disease progression and CD4+ lymphocyte depletion in 53 HIV-1-infected, asymptomatic individuals. MT-2-negative viruses were isolated from 49% of the patients both early and late during the follow-up period; 38% converted from being MT-2 negative to MT-2 positive, while 11% were MT-2 positive throughout the study. One individual showed a fluctuating virus phenotype. The loss of CD4+ lymphocytes was significantly more rapid in MT-2-positive patients. We found a broad spectrum of CD4+ lymphocyte changes in patients whose virus changed its MT-2 tropism. Our data suggest that the changes could be divided into three general patterns. A stable or slowly decreasing CD4+ lymphocyte count changed into a more rapid fall in 44% of the patients, no significant change in rate of decline could be noted in 44% of the patients, while a stable CD4+ lymphocyte level after a change in MT-2 tropism was noted in 12% of the patients. A correlation between MT-2 tropism and clinical symptoms was also noted. Half of the patients with MT-2-negative virus throughout the study were still asymptomatic after a mean follow-up time of 80 months, while only 15% of those who converted remained asymptomatic. All patients with MT-2-positive viruses at the time of inclusion in the study developed HIV-1-related symptoms, and half of them died during the study. The MT-2 status of 16 patients, could be determined at the time of AIDS diagnosis; 50% were Mt-2 positive, while 50% were MT-2 negative. No difference in AIDS-defining diagnoses or CD4+ lymphocyte counts at the time of diagnosis was noted. Knowledge of the HIV-1 phenotype may improve the early recognition of progressive disease.
机译:研究了人类免疫缺陷病毒1型(HIV-1)分离株在MT-2细胞中复制的能力,作为53个HIV-1感染无症状个体中疾病进展和CD4 +淋巴细胞耗竭的预后标志物。在随访期间的早期和晚期,从49%的患者中分离出MT-2阴性病毒。在整个研究过程中,有38%从MT-2阴性转变为MT-2阳性,而11%是MT-2阳性。一个人表现出波动的病毒表型。 MT-2阳性患者中CD4 +淋巴细胞的损失明显更快。我们发现在病毒改变其MT-2向性的患者中,CD4 +淋巴细胞变化范围广。我们的数据表明,这些变化可以分为三种一般模式。稳定或缓慢减少的CD4 +淋巴细胞计数在44%的患者中变为更快的下降,在44%的患者中未观察到下降率的显着变化,而MT-改变后CD4 +淋巴细胞水平稳定在12%的患者中发现2嗜性。还指出了MT-2向性与临床症状之间的相关性。在整个研究期间,平均随访80个月后,一半的MT-2阴性病毒患者仍无症状,而仅15%的转化患者仍无症状。在纳入研究时,所有患有MT-2阳性病毒的患者都出现了HIV-1相关症状,其中一半在研究期间死亡。在诊断AIDS时可以确定16例患者的MT-2状况; 50%的Mt-2阳性,而50%的MT-2阴性。在诊断时没有发现艾滋病定义诊断或CD4 +淋巴细胞计数的差异。对HIV-1表型的了解可能会改善对疾病进展的早期认识。

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