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Characterization of the HIV-1 transcription profile after romidepsin administration in ART-suppressed individuals

机译:在艺术抑制个体中romidepsin施用后HIV-1转录简谱的表征

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摘要

Supplemental Digital Content is available in the text Objectives: Reversing HIV-1 latency has been suggested as a strategy to eradicate HIV-1. We investigated the effect of romidepsin on the HIV transcription profile in participants from the REDUC part B clinical trial. Design: Seventeen participants on suppressive antiretroviral therapy were vaccinated with six doses of the therapeutic vaccine Vacc-4x followed by treatment with three doses of romidepsin. Samples from nine study participants were available for HIV transcription profile analysis. Methods: Read-through, total (TAR), elongated (longLTR), polyadenylated (polyA) and multiply-spliced (Tat-Rev) HIV transcripts and total HIV DNA were quantified at baseline (visit 1) and 4?h after the second (visit 10b) and third (visit 11b) romidepsin infusions. Results: Read-through, total, elongated, and polyadenylated HIV transcripts increased after romidepsin infusion ( P ?=?0.020, P ?=?0.0078, P ?=?0.0039, P ?=?0.027, respectively), but no changes were observed in multiply-spliced HIV RNA or HIV DNA. No change was observed in the ratio of read-through/total HIV transcripts. The ratio of elongated/total HIV RNA increased after romidepsin ( P ?=?0.016), whereas the ratio of polyadenylated/elongated HIV decreased. Both elongated HIV transcripts and total HIV DNA correlated negatively with the time to viral rebound after interruption of ART. Conclusions: In these patients, romidepsin increased early events in HIV transcription (initiation and especially elongation), but had less effect on later stages (completion, multiple splicing) that may be required for comprehensive latency reversal and cell killing. Without cell death, increased HIV transcription before or after latency reversal may hasten viral rebound after therapy interruption.
机译:文本目标中提供了补充数字内容:逆转HIV-1延迟被建议作为根除HIV-1的策略。我们调查了Romidepsin对Reduc Part临床试验的参与者中的HIV转录简易员的影响。设计:抑制抗逆转录病毒治疗的十七位参与者用六剂治疗疫苗Vacc-4x接种接种,然后用三个剂量的Romidepsin治疗。来自九项研究参与者的样本可用于HIV转录简介分析。方法:通过基线(参见1)和4μm (访问10B)和第三(访问11B)Romidepsin输注。结果:ROMIDESIN输注后读数,总,细长和聚酰胺化HIV转录物(P?= 0.020,P?= 0.0078,P?= 0.0039,P?=?0.027),但没有变化观察到乘以剪接的HIV RNA或HIV DNA。在接通/总HIV转录物的比例中没有观察到任何变化。在ROMIDESIN后,细长/总HIV RNA的比例增加(P?= 0.016),而聚腺苷酸/细长艾滋病毒的比例降低。随着艺术中断后,细长的HIV转录物和总HIV DNA与病毒反弹的时间负相关。结论:在这些患者中,Romidepsin增加了HIV转录的早期事件(开始,特别是伸长),但对综合潜伏期和细胞杀伤可能需要的后期阶段(完整,多剪接)的影响较小。没有细胞死亡,在治疗中断后,延迟逆转之前或之后增加了艾滋病毒转录可能会加速病毒反弹。

著录项

  • 来源
    《AIDS》 |2019年第3期|共7页
  • 作者单位

    San Francisco Veterans Affairs (VA) Medical Center and University of California San Francisco (UCSF);

    San Francisco Veterans Affairs (VA) Medical Center and University of California San Francisco (UCSF);

    The Department of Infectious Diseases Aarhus University Hospital;

    The Department of Infectious Diseases Aarhus University Hospital;

    San Francisco Veterans Affairs (VA) Medical Center and University of California San Francisco (UCSF);

    San Francisco Veterans Affairs (VA) Medical Center and University of California San Francisco (UCSF);

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 传染病;
  • 关键词

    HIV-1; humans; latency; RNA; RNA splicing; romidepsin; transcription;

    机译:HIV-1;人类;潜伏期;RNA;RNA拼接;ROMITEPSIN;转录;

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