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HIV 共感染中的单个肝细胞乙型肝炎病毒转录景观。

Single Hepatocyte Hepatitis B Virus Transcriptional Landscape in HIV Coinfection.

机构信息

Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

Virginia Commonwealth University Health System, Richmond, Virginia, USA.

出版信息

J Infect Dis. 2020 Apr 7;221(9):1462-1469. doi: 10.1093/infdis/jiz607.

DOI:10.1093/infdis/jiz607
PMID:31740931
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7137881/
Abstract

BACKGROUND

Hepatitis B virus (HBV) is a leading cause of liver failure and hepatocellular carcinoma. Approximately 10% of people with HIV also have HBV and are at higher risk of liver disease progression than in HBV monoinfection. Antivirals, common to HIV and HBV, suppress HBV DNA levels but do not eradicate virus because the transcriptional template, covalently closed circular DNA (cccDNA), is long lived in infected hepatocytes.

METHODS

Using single-cell laser capture microdissection, we isolated >1100 hepatocytes from 5 HIV/HBV coinfected persons with increasing exposure to HBV antivirals (HB1-HB5; no exposure to >7 years exposure), quantifying cccDNA and pregenomic RNA (pgRNA) in each cell using droplet digital polymerase chain reaction.

RESULTS

The proportion of infected hepatocytes decreased with antiviral exposure from 96.4% (HB1) to 29.8% (HB5). Upper cccDNA range and median pgRNA decreased from HB1 to HB5 (P < .05 for both). The amount of pgRNA transcribed per cccDNA also decreased from HB1 to HB5 (P < .05). Cells with inactive pgRNA transcription were enriched from 0% (HB1) to 14.3% (HB5) of infected hepatocytes.

CONCLUSIONS

cccDNA transcription is reduced in HIV/HBV coinfected people with longer antiviral duration. Understanding HBV transcriptional regulation may be critical to develop a functional cure.

摘要

背景

乙型肝炎病毒 (HBV) 是导致肝功能衰竭和肝细胞癌的主要原因。约 10%的 HIV 感染者同时感染 HBV,并且比 HBV 单感染患者更容易发生肝病进展。抗 HIV 和 HBV 的常用抗病毒药物可抑制 HBV DNA 水平,但不能根除病毒,因为感染肝细胞中的转录模板共价闭合环状 DNA (cccDNA) 寿命较长。

方法

我们使用单细胞激光捕获显微切割技术,从 5 名 HIV/HBV 合并感染的个体中分离出 >1100 个肝细胞,这些个体的 HBV 抗病毒药物暴露程度逐渐增加(HB1-HB5;未>7 年暴露),使用液滴数字聚合酶链反应在每个细胞中定量检测 cccDNA 和前基因组 RNA (pgRNA)。

结果

随着抗病毒药物暴露时间的增加,感染肝细胞的比例从 96.4%(HB1)下降到 29.8%(HB5)。HB1 到 HB5 的 cccDNA 上限和中位 pgRNA 减少(均 P <.05)。每个 cccDNA 转录的 pgRNA 量也从 HB1 到 HB5 减少(P <.05)。无活性 pgRNA 转录的细胞从 HB1 时的 0%(HB1)富集到 HB5 时的 14.3%(HB5)。

结论

抗病毒治疗时间越长,HIV/HBV 合并感染患者的 cccDNA 转录减少。了解 HBV 转录调控对于开发功能性治愈可能至关重要。

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