Classification and sequencing of hepatitis D virus from a large cohort of chronically infected individuals paired with co-infecting hepatitis B virus sequencing: a genomic characterisation study.

IF 20.4 1区生物学 Q1 INFECTIOUS DISEASES

Lancet Microbe Pub Date : 2026-04-09 DOI:10.1016/j.lanmic.2025.101328

Savrina Manhas, Silvia Chang, Ross Martin, Andrew Lopez, Thomas Aeschbacher, Simin Xu, Roberto Mateo, Yang Liu, Stephanie Narguet, Dzhamal Abdurakhmanov, Pietro Lampertico, Dmitry Manuilov, John Flaherty, Hongmei Mo, Evguenia Maiorova, Tarik Asselah

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引用次数: 0

Abstract

Background: The most severe form of viral hepatitis is caused by co-infection of hepatitis D virus (HDV) and hepatitis B virus (HBV). Phylogenetic analyses classify HBV and HDV into eight major genotypes: HBV GTA to GTH and HDV GT1 to GT8. Paired HBV and HDV sequencing data from participants with chronic hepatitis delta are scarce. We aimed to sequence and genotype HDV and HBV from a large cohort of participants from clinical studies and diverse countries of origin.

Methods: 407 participants with chronic hepatitis D from 24 countries were characterised (124 participants from MYR301 clinical trial, 93 from MYR204, 114 from MYR202, and an additional 76 participants from diverse geographical locations). HBV and HDV from participants were analysed using sequencing, enzyme immunoassay, or both to determine HBV and HDV genotypes. BLAST analysis and phylogenetics were used to determine HBV and HDV genotypes with reference sequence libraries. Bulevirtide treatment response (measured by HDV RNA decline and normalisation of alanine aminotransferase) was compared by genotype for MYR trial participants.

Findings: HDV sequencing assays were successful for 386 (95%) of 407 participants and HBV sequencing or serology-based HBV genotyping assays were successful for genotyping 395 (97%) participants. For individual genotypes, HBV GTD (336 [83%] participants) and HDV GT1 (364 [89%]) were the most prevalent. For paired HBV-HDV genotypes, HBV-HDV D/1 was most common (320 [79%] of 407) followed by A/1 (30 [7%]). Phylogenetic analyses of HDV full-genome sequences showed distinct clusters of sequences within HDV GT1, and four novel provisional HDV GT1 subgenotypes, HDV GT1fp to HDVGT1ip, were identified. For 218 MYR clinical trial participants, bulevirtide treatment response was similar across HDV GT1 subgenotypes (both established and newly identified).

Interpretation: Novel HDV subgenotypes identified in this study indicate a greater genetic diversity of HDV GT1 than previously recognised. This knowledge will be important for developing better diagnostics, and in understanding HDV genotype-specific biology and response to treatment. More extensive HDV sequencing from under-sampled regions, such as Africa, is needed to determine the true breadth of HDV sequence and genotype diversity.

Funding: Gilead Sciences.

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从大量慢性感染个体配对的同时感染乙型肝炎病毒的丁型肝炎病毒的分类和测序：一项基因组特征研究

背景：最严重的病毒性肝炎是由丁型肝炎病毒（HDV）和乙型肝炎病毒（HBV）共同感染引起的。系统发育分析将HBV和HDV分为8个主要基因型：HBV GTA至GTH和HDV GT1至GT8。来自慢性丁型肝炎患者的配对HBV和HDV测序数据很少。我们的目的是从临床研究和不同原产国的大量参与者中对HDV和HBV进行测序和基因分型。方法：对来自24个国家的407名慢性丁型肝炎患者进行了研究（124名来自MYR301临床试验，93名来自MYR204, 114名来自MYR202，另外76名来自不同地理位置的参与者）。使用测序、酶免疫测定或两者同时分析来自参与者的HBV和HDV，以确定HBV和HDV基因型。利用BLAST分析和系统发育方法，利用参考序列文库确定HBV和HDV基因型。对MYR试验参与者的布来韦肽治疗反应（通过HDV RNA下降和丙氨酸转氨酶正常化来测量）进行基因型比较。结果：407名参与者中有386人（95%）的HDV测序检测成功，395名（97%）参与者的HBV测序或基于血清学的HBV基因分型检测成功。就个体基因型而言，HBV GTD（336[83%]名参与者）和HDV GT1（364[89%]名参与者）最为普遍。对于配对的HBV-HDV基因型，HBV-HDV D/1最常见（407例中320例[79%]），其次是A/1（30例[7%]）。对HDV全基因组序列的系统发育分析显示，在HDVGT1中存在明显的序列簇，并鉴定出HDV GT1fp至HDVGT1ip四个新的临时HDVGT1亚基因型。在218名MYR临床试验参与者中，布来韦肽的治疗反应在不同的HDV GT1亚基因型（包括已建立的和新发现的）中是相似的。解释：在这项研究中发现的新的HDV亚基因型表明，HDV GT1的遗传多样性比以前认识到的要大。这一知识对于开发更好的诊断方法以及了解HDV基因型特异性生物学和对治疗的反应非常重要。需要从非洲等取样不足的地区进行更广泛的HDV测序，以确定HDV序列的真正广度和基因型多样性。资助：Gilead Sciences。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Lancet Microbe Multiple-

CiteScore

27.20

自引率

0.80%

发文量

278

审稿时长

6 weeks

期刊介绍： The Lancet Microbe is a gold open access journal committed to publishing content relevant to clinical microbiologists worldwide, with a focus on studies that advance clinical understanding, challenge the status quo, and advocate change in health policy.