首页> 外文期刊>Scandinavian journal of immunology. >Relevance of CD38 expression on CD8 T cells to evaluate antiretroviral therapy response in HIV-1-infected youths.
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Relevance of CD38 expression on CD8 T cells to evaluate antiretroviral therapy response in HIV-1-infected youths.

机译:CD38 T细胞上CD38表达的相关性以评估HIV-1感染青年的抗逆转录病毒疗法反应。

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Surrogate markers for monitoring immuno-virological discordant responders, in addition to plasma viral load and CD4 cells, are still lacking. We assessed the diagnostic utility of CD38 expression on CD8 T cell assay, alone or in association with lymphocyte proliferation to mycotic antigens, in evaluating antiretroviral response. 28 vertically HIV-infected youths, 21 HAART- and seven 2 nucleotide reverse transcriptase inhibitors-treated, were enrolled in a retrospective study. Responders (57.1%) and non-responders (42.9%) to stable antiretroviral therapy for a minimum of 6 months, on the basis of viral load and CD4 T cells, comprehensively evaluated by CD38 expression on CD8 T lymphocytes [measured as CD38 antibody bound per CD8 T cell (CD38 ABC) and %CD38+ of total CD8 T cells (%CD38/CD8)] and lymphocyte proliferation to P. jiroveci, C. albicans, C. neoformans, A. fumigatus at a single time point after treatment, were selected. CD38 expression > or =2401 CD38 ABC and > or =85% CD38/CD8 cut-off points, accurately discriminates responders versus non-responders, both measures resulting in 75.0% (CI 42.8-94.5) sensitivity (identification of non-responder) and 93.8% (CI 69.8-99.8) specificity (identification of responder), when considered as single assays. The association '> or =2401 CD38 ABC or > or =85% CD38/CD8' improved sensitivity to 83.3% (CI 51.6-97.9), while the association '<2401 CD38ABC (or <85% CD38/CD8) and lymphoproliferative response positive to > or =2 tested organisms' improved specificity to 100% (CI 79.4-100). In conclusions, CD38 expression and mycotic antigen-specific T-cell proliferation may be used as additional parameters to existing criteria to evaluate antiretroviral response in immuno-virological discordant patients.
机译:除了血浆病毒载量和CD4细胞外,仍缺乏用于监测免疫-病毒学不一致反应者的替代标记。我们评估了CD38 T细胞分析中CD38表达的诊断效用,单独或与淋巴细胞对真菌抗原的增殖有关,以评估抗逆转录病毒应答。一项回顾性研究纳入了28名垂直感染HIV的青年,21名HAART和7种2核苷酸逆转录酶抑制剂的治疗。响应者(57.1%)和无响应者(42.9%)在稳定的抗逆转录病毒治疗至少6个月的基础上,根据病毒载量和CD4 T细胞,通过CD8 T淋巴细胞上CD38的表达进行了全面评估[测量为结合CD38抗体每个CD8 T细胞(CD38 ABC)和总CD8 T细胞的%CD38 +(%CD38 / CD8)],并在治疗后的单个时间点将淋巴细胞增殖至毕氏疟原虫,白色念珠菌,新孢梭菌,烟曲霉,被选中。 CD38表达>或= 2401 CD38 ABC和>或= 85%CD38 / CD8临界点,可准确地区分响应者与非响应者,两种方法均产生75.0%(CI 42.8-94.5)的敏感性(识别非响应者)当被认为是单一测定法时,具有93.8%(CI 69.8-99.8)的特异性(鉴定反应者)。关联'>或= 2401 CD38 ABC或>或= 85%CD38 / CD8'将敏感性提高到83.3%(CI 51.6-97.9),而关联'<2401 CD38ABC(或<85%CD38 / CD8)和淋巴增生反应对大于或等于2个测试有机体呈阳性的特异性提高到100%(CI 79.4-100)。总之,CD38表达和真菌抗原特异性T细胞增殖可以用作现有标准的附加参数,以评估免疫-病毒学不一致患者的抗逆转录病毒应答。

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