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Antigen-responsive CD4 + T cell clones contribute to the HIV-1 latent reservoir

机译:抗原响应性CD4 + T细胞克隆有助于HIV-1潜储层

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Mendoza et al. identify clones of HIV-1 defective or intact latent proviruses within antigen-responsive CD4 ~(+) T cells. This study suggests that exposure to chronic or recurrent antigens may contribute to reservoir persistence by stimulating the clonal expansion of latently infected CD4 ~(+) T cells. Antiretroviral therapy suppresses but does not cure HIV-1 infection due to the existence of a long-lived reservoir of latently infected cells. The reservoir has an estimated half-life of 44 mo and is largely composed of clones of infected CD4 ~(+) T cells. The long half-life appears to result in part from expansion and contraction of infected CD4 ~(+) T cell clones. However, the mechanisms that govern this process are poorly understood. To determine whether the clones might result from and be maintained by exposure to antigen, we measured responses of reservoir cells to a small subset of antigens from viruses that produce chronic or recurrent infections. Despite the limited panel of test antigens, clones of antigen-responsive CD4 ~(+) T cells containing defective or intact latent proviruses were found in seven of eight individuals studied. Thus, chronic or repeated exposure to antigen may contribute to the longevity of the HIV-1 reservoir by stimulating the clonal expansion of latently infected CD4 ~(+) T cells.
机译:Mendoza等。鉴定抗原响应CD4〜(+)T细胞内的HIV-1缺陷或完整的潜在潜伏的克隆。该研究表明,暴露于慢性或复发性抗原可以通过刺激潜伏的CD4〜(+)T细胞的克隆膨胀来促进储层持久性。抗逆转录病毒疗法抑制但由于存在潜伏的潜伏的细胞的长期储层而无法治愈HIV-1感染。储存器估计的44Mo半衰期,并且主要由受感染的CD4〜(+)T细胞的克隆组成。长半衰期似乎部分地导致感染的CD4〜(+)T细胞克隆的膨胀和收缩。然而,管理该过程的机制被理解得很差。为了确定克隆是否可以通过暴露于抗原来维持,我们测量储层细胞对产生慢性或反复感染的病毒的小抗原的副群的反应。尽管有限的试验抗原面板有限,但抗原响应CD4〜(+)T细胞的克隆含有有缺陷或完整的潜水潜水术中的七个中的七个中的七个。因此,通过刺激潜伏的CD4〜(+)T细胞的克隆膨胀,慢性或反复暴露于抗原可能有助于HIV-1储存器的寿命。

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