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慢性乙型肝炎病毒感染的黑猩猩和接受ARC-520 siRNA治疗的患者中乙型肝炎病毒转录本的特征表明cccDNA的转录沉默。

Characterization of Hepatitis B Virus Transcripts in Chronically HBV-Infected Chimpanzees and Patients Treated with ARC-520 siRNA Demonstrates Transcriptional Silencing of cccDNA.

作者信息

Wooddell Christine I, Sanders Dean, Xu Zhao, Mak Lung-Yi, Schluep Thomas, Seto Wai-Kay, Given Bruce D, Yuen Man-Fung

机构信息

Arrowhead Pharmaceuticals Inc., 502 S. Rosa Road, Madison, WI 53719, USA.

Arrowhead Pharmaceuticals Inc., 10102 Hoyt Park Drive, San Diego, CA 92131, USA.

出版信息

Viruses. 2024 Dec 19;16(12):1943. doi: 10.3390/v16121943.

Abstract

Full-length hepatitis B virus (HBV) transcripts of chimpanzees and patients treated with multidose (MD) HBV siRNA ARC-520 and entecavir (ETV) were characterized by single-molecule real-time (SMRT) sequencing, identifying multiple types of transcripts with the potential to encode HBx, HBsAg, HBeAg, core, and polymerase, as well as transcripts likely to be derived from dimers of dslDNA, and these differed between HBeAg-positive (HBeAg+) and HBeAg-negative (HBeAg-) individuals. HBV transcripts from the last follow-up ~30 months post-ARC-520 treatment were categorized from one HBeAg+ (one of two previously highly viremic patients that became HBeAg- upon treatment and had greatly reduced cccDNA products) and four HBeAg- patients. The previously HBeAg+ patient received a biopsy that revealed that he had 3.4 copies/cell cccDNA (two to three orders of magnitude more cccDNA than HBeAg- chimpanzees) but expressed primarily truncated X and HBsAg from iDNA, like two patients that were HBeAg- at the start of the study and had one copy/cell cccDNA. No HBV transcripts were detected in two other HBeAg- patients that had ~0.3 copies/cell cccDNA, one of which had seroconverted for HBsAg. The paucity of cccDNA-derived transcripts in the presence of high cccDNA demonstrates the transcriptional silencing of HBV following MD siRNA treatment with ETV.

摘要

通过单分子实时(SMRT)测序对接受多剂量(MD)乙肝病毒(HBV)小干扰RNA(siRNA)ARC-520和恩替卡韦(ETV)治疗的黑猩猩及患者的全长HBV转录本进行了表征,鉴定出多种可能编码HBx、HBsAg、HBeAg、核心蛋白和聚合酶的转录本类型,以及可能源自双链松弛环状DNA(dslDNA)二聚体的转录本,并且这些转录本在HBeAg阳性(HBeAg+)和HBeAg阴性(HBeAg-)个体之间存在差异。对ARC-520治疗后约30个月的最后一次随访中的HBV转录本进行分类,来自1例HBeAg+患者(之前两名高病毒血症患者之一,治疗后变为HBeAg-且cccDNA产物大幅减少)和4例HBeAg-患者。之前的HBeAg+患者接受了活检,结果显示其细胞中cccDNA含量为3.4拷贝/细胞(比HBeAg-黑猩猩的cccDNA多两到三个数量级),但主要从整合DNA(iDNA)表达截短的X蛋白和HBsAg,这与研究开始时为HBeAg-且细胞中cccDNA含量为1拷贝/细胞的两名患者情况类似。在另外两名细胞中cccDNA含量约为0.3拷贝/细胞的HBeAg-患者中未检测到HBV转录本,其中1例已发生HBsAg血清学转换。在存在高含量cccDNA的情况下,cccDNA衍生转录本的缺乏表明MD siRNA联合ETV治疗后HBV发生了转录沉默。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ecb/11680220/8e1d021d6d4e/viruses-16-01943-g001.jpg

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