表达与病毒中和相关的变异 IGHV1-69 编码抗原受体的 B 细胞在慢性 HCV 感染患者中显示出淋巴瘤样转录组。

IF 5.6 2区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Hepatology Communications Pub Date : 2024-07-31 eCollection Date: 2024-08-01 DOI:10.1097/HC9.0000000000000503
Christoph Schultheiß, Edith Willscher, Lisa Paschold, Christin Ackermann, Moritz Escher, Rebekka Scholz, Maximilian Knapp, Jana Lützkendorf, Lutz P Müller, Julian Schulze Zur Wiesch, Mascha Binder
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引用次数: 0

摘要

背景:慢性丙型肝炎病毒感染会导致适应性免疫细胞发生复杂的相互作用,从而可能导致B细胞异常,如冷球蛋白血症或淋巴瘤。虽然直接作用抗病毒疗法降低了严重肝损伤的发生率,但其对肝外 HCV 表现(如 B 细胞异常)的影响仍不明确:我们对慢性HCV单一感染患者和经直接作用抗病毒治疗后获得持续病毒学应答(SVR)的HCV患者的B细胞受体(BCR)序列进行了测序。该数据集用于挖掘高度中和的HCV抗体,并与弥漫性大B细胞淋巴瘤数据集进行比较。TKO模型用于测试体外选定B-BCR的信号转导强度。对慢性HCV和HCV SVR样本进行了单细胞RNA测序,以分析具有HCV中和抗原受体的B细胞转录组:结果:我们在慢性HCV和SVR患者中发现了具有高丰富度和体细胞高突变的B细胞指纹。与特异性免疫球蛋白基因的汇聚产生了高连接性互补决定区 3 网络。此外,我们还观察到,IGHV1-69 CDR1和FR3突变具有高度中和HCV抗体的特征,与高级别淋巴瘤克隆型BCR中发现的复发性点突变相对应。在用于评估 BCR 信号强度的体外细胞模型中,这些 BCR 没有显示出自主信号传导,但激活阈值较低。单细胞 RNA 测序显示,携带这些点突变的 B 细胞显示出持续的致癌转录组特征,信号节点(如 CARD11、MALT1、RelB、MAPK 和 NFAT)失调:我们提供的证据表明,淋巴瘤样细胞来源于抗 HCV 免疫反应。在许多患者中,这些细胞在 SVR 后持续存在多年,可以被解释为 HCV 相关 B 细胞异常和淋巴瘤风险增加的机理基础,甚至在病毒消除后也是如此。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
B cells expressing mutated IGHV1-69-encoded antigen receptors related to virus neutralization show lymphoma-like transcriptomes in patients with chronic HCV infection.

Background: Chronic HCV infection leads to a complex interplay with adaptive immune cells that may result in B cell dyscrasias like cryoglobulinemia or lymphoma. While direct-acting antiviral therapy has decreased the incidence of severe liver damage, its effect on extrahepatic HCV manifestations such as B cell dyscrasias is still unclear.

Methods: We sequenced B cell receptor (BCR) repertoires in patients with chronic HCV mono-infection and patients with HCV with a sustained virological response (SVR) after direct-acting antiviral therapy. This data set was mined for highly neutralizing HCV antibodies and compared to a diffuse large B cell lymphoma data set. The TKO model was used to test the signaling strength of selected B-BCRs in vitro. Single-cell RNA sequencing of chronic HCV and HCV SVR samples was performed to analyze the transcriptome of B cells with HCV-neutralizing antigen receptors.

Results: We identified a B cell fingerprint with high richness and somatic hypermutation in patients with chronic HCV and SVR. Convergence to specific immunoglobulin genes produced high-connectivity complementarity-determining region 3 networks. In addition, we observed that IGHV1-69 CDR1 and FR3 mutations characterizing highly neutralizing HCV antibodies corresponded to recurrent point mutations found in clonotypic BCRs of high-grade lymphomas. These BCRs did not show autonomous signaling but a lower activation threshold in an in vitro cell model for the assessment of BCR signaling strength. Single-cell RNA sequencing revealed that B cells carrying these point mutations showed a persisting oncogenic transcriptome signature with dysregulation in signaling nodes such as CARD11, MALT1, RelB, MAPK, and NFAT.

Conclusions: We provide evidence that lymphoma-like cells derive from the anti-HCV immune response. In many patients, these cells persist for years after SVR and can be interpreted as a mechanistic basis for HCV-related B cell dyscrasias and increased lymphoma risk even beyond viral elimination.

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来源期刊
Hepatology Communications
Hepatology Communications GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
8.00
自引率
2.00%
发文量
248
审稿时长
8 weeks
期刊介绍: Hepatology Communications is a peer-reviewed, online-only, open access journal for fast dissemination of high quality basic, translational, and clinical research in hepatology. Hepatology Communications maintains high standard and rigorous peer review. Because of its open access nature, authors retain the copyright to their works, all articles are immediately available and free to read and share, and it is fully compliant with funder and institutional mandates. The journal is committed to fast publication and author satisfaction. ​
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