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HIV-1 viruses detected during episodic blips following interleukin-7 administration are similar to the viruses present before and after interleukin-7 therapy.

机译:在施用白介素7之后的发作性斑点期间检测到的HIV-1病毒与白介素7治疗之前和之后存在的病毒相似。

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BACKGROUND: administration of recombinant human interleukin (IL)-7 leads to CD4 and CD8 T-cell expansions in HIV-infected individuals, demonstrating promising capacity for immune reconstitution. However, a proportion of patients treated with recombinant human IL-7 experience transient increases in plasma HIV-RNA ('blips'), possibly reflecting 'purging' of a quiescent reservoir that provides a barrier to viral eradication. OBJECTIVE: to identify the sources of HIV detected during transient viremic episodes following IL-7 administration, viral quasispecies were analyzed in a total of 281 primary sequences derived from seven patients who experienced the episodic blips following IL-7 therapy. METHOD: the C2-V3 regions of the HIV-1 env gene were sequenced from HIV-1 RNA in plasma and HIV DNA from peripheral blood mononuclear cells (PBMCs) obtained at baseline (day 0 of recombinant human IL-7 therapy), during the episode of viral blips (day 4), and at a time when levels of plasma HIV-RNA had returned to less than 50 copies/ml (day 28). RESULTS: the HIV sequences detected during transient viremia following IL-7 administration were closely related to those of the plasma viruses present before and after cytokine administration. All virus quasispecies detected during blips were also present in proviral sequences in PBMCs. CONCLUSION: the low level viremia induced by IL-7 likely reflects predominantly transient induction or release of virus from a preexisting pool rather than activation of silent quasispecies.
机译:背景:重组人白介素(IL)-7的使用导致HIV感染者体内CD4和CD8 T细胞的扩增,证明了免疫重建的潜力。但是,接受重组人IL-7治疗的患者中,有一部分患者的血浆HIV-RNA出现短暂增加(“斑点”),这可能反映出“清除”了一个静止的贮液池,为消除病毒提供了障碍。目的:为了鉴定在IL-7给药后短暂病毒血症发作期间检测到的HIV来源,分析了共计281个主要序列的病毒准种,这些序列来自7名在IL-7治疗后经历过短暂发作的患者。方法:从基线(重组人IL-7治疗第0天)获得的血浆HIV-1 RNA和外周血单个核细胞(PBMC)的HIV DNA的HIV-1 env基因的C2-V3区域进行测序。病毒斑点发作(第4天),以及血浆HIV-RNA水平降至低于50拷贝/ ml(第28天)的时间。结果:IL-7给药后在短暂病毒血症期间检测到的HIV序列与细胞因子给药前后存在的血浆病毒序列密切相关。斑点期间检测到的所有病毒准种也存在于PBMC中的前病毒序列中。结论:IL-7诱导的低水平病毒血症可能主要反映了病毒从先前存在的库中短暂地诱导或释放,而不是沉默的准种的激活。

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