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http://dx.doi.org/10.25673/117987| Title: | B cells expressing mutated IGHV1-69-encoded antigen receptors related to virus neutralization show lymphoma-like transcriptomes in patients with chronic HCV infection |
| Author(s): | Schultheiß, Christoph Willscher, Edith Paschold, Lisa Ackermann, Christin Escher, Moritz Scholz, Rebekka Knapp, Maximilian Lützkendorf, Jana Müller, Lutz P. Schulze zur Wiesch, Julian Constantin Raimar Binder, Mascha |
| Issue Date: | 2024 |
| Type: | Article |
| Language: | English |
| Abstract: | 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. Abstract |
| URI: | https://opendata.uni-halle.de//handle/1981185920/119947 http://dx.doi.org/10.25673/117987 |
| Open Access: |  Open access publication |
| License: |  (CC BY 4.0) Creative Commons Attribution 4.0 |
| Journal Title: | Hepatology communications |
| Publisher: | Wolters Kluwer Health |
| Publisher Place: | [Alphen aan den Rijn] |
| Volume: | 8 |
| Issue: | 8 |
| Original Publication: | 10.1097/HC9.0000000000000503 |
| Page Start: | 1 |
| Page End: | 15 |
| Appears in Collections: | Open Access Publikationen der MLU |
Files in This Item:
| File | Description | Size | Format | |
|---|---|---|---|---|
| b_cells_expressing_mutated_ighv1_69_encoded.19.pdf | 4.17 MB | Adobe PDF |  View/Open |