HIV潜伏期和独特的解剖储存库:一项系统综述

Satyendra Prakash, Ramendra K. Singh
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引用次数: 0

摘要

虽然HAART(高活性抗逆转录病毒疗法)药物的三重形式成倍提高CD4+ T免疫细胞计数在HIV-1感染的患者,并提高了许多HIV-1感染的患者的预期寿命。药物研究结果也有助于将HIV-1感染患者的血浆病毒载量提高到临床无法检测的水平。然而,通过这些药物干预,完全根除或治疗病毒是很难实现的。提出的主要障碍是宿主CD4+ T免疫细胞内持续进行的病毒复制。这些被感染的免疫细胞可以转化为潜伏期(转录沉默)多年,并且很难被当前基于haart的干预措施所靶向。除了HIV-1病毒的这个令人难以置信的特性,它还可以简单地隐藏在不同的解剖储存库中,这些储存库在不同的位置有免疫细胞。这些位点的存在很容易使病毒逃避宿主的免疫监视,也有助于在接受抗逆转录病毒治疗的患者中产生低病毒。因此,我们回顾了目前的知识,以便更好地理解HIV-1潜伏期建立过程中的多因素机制,并进行了大量实验研究,这些实验研究强烈支持正在进行的病毒复制和在不同解剖储存库中的持久性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
HIV Latency and Distinct Anatomical Reservoirs: A Systemic Review
Although the HAART (Highly Active Antiretroviral Therapy) a triple form of drugs has exponentially enhanced the CD4+ T immune cell count in HIV-1 infected patients and has improved the expectancy of many HIV-1 infected patients’ life. The drug results have also contributed to bringing the plasma virus load up to a clinically undetectable level in HIV-1 infected patients for several years. However, with these drug interventions, complete eradication or treatment of the virus is hard to achieve. The primary obstacle that has been raised is the persistence of ongoing viral replication inside the host CD4+ T immune cells. These infected immune cells can be transformed into the latent stage (transcriptionally silent) for many years and hardly be targeted by the current HAART-based interventions. Besides this incredible specialty of the HIV-1 virus, it can also simply hide in diverse anatomical reservoirs having immune cells at separated locations. The presence of these locations easily facilitates the virus to escape from the host immune surveillance and also contributes to low viral production in patients on antiretroviral therapy. As a result, we review our current knowledge to provide a better understanding of multifactorial mechanisms during the establishment of HIV-1 latency with numerous experimental studies that strongly uphold the ongoing viral replication and persistence at the distinct anatomical reservoirs.
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