T-cell dysfunction in HIV-1 infection: targeting the inhibitors

HIV therapy Pub Date : 2010-01-01 DOI:10.2217/HIV.09.51
J. Downey, N. Imami
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引用次数: 5

Abstract

Since AIDS emerged almost three decades ago, there have been considerable advances in the field of antiretroviral chemotherapy for those chronically infected with HIV-1. However, this therapy is noncurative and as our understanding of HIV-1 immunopathogenesis increases, it is becoming apparent that further therapeutic interventions are required to reverse the devastating effects of HIV-1 infection worldwide. While viral clearance remains the principle goal of HIV-1 treatment, this article describes immunotherapeutic options that target the immunological effects of the virus, to reduce its presence in the body and counteract viral-induced T-cell dysfunction and inhibition. Such approaches may augment existing antiretroviral therapy to overturn virus-induced T-cell anergy in the infected host, improving levels of immune control that reduce viremia and decrease the rate of transmission.
HIV-1感染中的t细胞功能障碍:靶向抑制剂
自从艾滋病在近30年前出现以来,针对慢性HIV-1感染者的抗逆转录病毒化疗领域取得了相当大的进展。然而,这种疗法是不可治愈的,随着我们对HIV-1免疫发病机制的了解的增加,很明显,需要进一步的治疗干预来扭转全世界HIV-1感染的破坏性影响。虽然病毒清除仍然是HIV-1治疗的主要目标,但本文描述了针对病毒免疫效应的免疫治疗选择,以减少其在体内的存在并抵消病毒诱导的t细胞功能障碍和抑制。这些方法可能会增强现有的抗逆转录病毒疗法,以逆转受感染宿主中病毒诱导的t细胞能量,提高免疫控制水平,从而减少病毒血症和降低传播率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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