首页> 外文期刊>The New Microbiologica >Immunovirological outcome and HIV-1 DNA decay in a small cohort of HIV-1-infected patients deintensificated from Abacavir/Lamivudine/Dolutegravir to Lamivudine plus Dolutegravir
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Immunovirological outcome and HIV-1 DNA decay in a small cohort of HIV-1-infected patients deintensificated from Abacavir/Lamivudine/Dolutegravir to Lamivudine plus Dolutegravir

机译:免疫病毒结果和HIV-1 DNA腐烂,在从Abacavir / Lamivudine / Dolutegravir到Lamivudine Plus DoluteGravir中致死的小群体的HIV-1感染患者中的DNA衰减

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Combination abacavir/lamivudine/dolutegravir (ABC/3TC/DTG) is approved as a first-line treatment for antiretroviral naive patients. This report investigated the immunovirological outcome and total HIV-1 DNA decay in a small cohort of nave HIV-1-positive patients treated with this regimen. In the presence of viral suppression and increased lymphocyte T CD4+ cells, the quantitative analysis of total HIV-1 DNA content revealed a significant decay after 12 months of treatment. Subsequently, we deintensificated the treatment of these patients from (ABC/3TC/DTG) to lamivudine plus dolutegravir (3TC/DTG) after 12 months of virological suppression, as a strategy of "induction-maintenance" therapy. The analysis of HIV-1 RNA viral load, total HIV-1 DNA, CD4+ T lymphocyte count and CD8+HLA-DR+ T lymphocyte percentage after a mean 3.5 months of therapy deintensification showed no significant difference with respect to data detected after 12 months of ABC/3TC/DTG treatment in the presence of continuous viral suppression. These results indicate that the deintensification of highly active antiretroviral therapy (HAART) from ABC/3TC/DTG to 3TC/DTG effectively controls HIV-1 replication and in the early period does not induce any significant variations of total HIV-1 DNA. This suggests that HAART deintensification might be proposed as a therapeutic evolution in the treatment of HIV-1 infection.
机译:组合Abacavir / Lamivudine / DoluteGravir(ABC / 3TC / DTG)被批准为抗逆转录病毒幼稚患者的一线治疗。本报告研究了免疫病毒结果和全部培养型纳维群核队列的免疫病毒结果和总HIV-1 DNA腐烂。在病毒抑制和增加的淋巴细胞T CD4 +细胞的存在下,总HIV-1 DNA含量的定量分析显示在治疗12个月后显着衰减。随后,我们将这些患者从(ABC / 3TC / DTG)视为在病毒学抑制12个月后从(ABC / 3TC / DTG)到Lamivudine Plus Dolutegravir(3TC / DTG),作为“诱导 - 维持”治疗的策略。 HIV-1 RNA病毒载荷的分析,总HIV-1 DNA,CD4 + T淋巴细胞计数和CD8 + HLA-DR + T淋巴细胞百分比后的疗法去活化后,对12个月后检测到的数据没有显着差异ABC / 3TC / DTG治疗在连续病毒抑制存在下。这些结果表明,从ABC / 3TC / DTG到3TC / DTG的高活性抗逆转录病毒治疗(HAART)的去敏化有效地控制了HIV-1复制,并且在早期不诱导总HIV-1 DNA的任何显着变化。这表明HAART Deintensification可能提出作为治疗HIV-1感染的治疗演变。

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