Biased IGH VDJ gene repertoire and clonal expansions in B cells of chronically hepatitis C virus–infected individuals

Tucci, Felicia Anna; Kitanovski, Simo; Johansson, Patricia; Klein-Hitpaß, Ludger; Kahraman, Alişan; Dürig, Jan; Hoffmann, Daniel; Küppers, Ralf

doi:10.1182/blood-2017-09-805762

Cited by 29 publications

(26 citation statements)

References 51 publications

(78 reference statements)

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“…Blum et al [102] identified preferential usage of certain IGHV segments in the plasmablast repertoires of Lyme disease patients. Tucci et al [103] reported disrupted B-cell repertoires in a cohort of chronic HCV patients due to preferential usage of several IGHV segments in IGM memory B-cells. While CDR3 may be conserved within a subset of antigen-specific sequences, even withinTCRs recognizing one epitope, there are frequently many distinct motifs, each successfully solving the task of antigen recognition [47,104].…”

Section: Clonal Sequence Featuresmentioning

confidence: 99%

T‐cell receptor and B‐cell receptor repertoire profiling in adaptive immunity

2019

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Summary B‐cell receptors and T‐cell receptors are the key molecules responsible for specific antigen recognition in adaptive immunity. The huge diversity of immune receptor repertoires constrained their comprehensive studies in the past. More recently, however, high‐throughput sequencing based techniques have revolutionized the field of immune receptor repertoire profiling enabling new insights into the development and function of the adaptive immune system. In this review we describe current methods for immune receptor profiling and software tools used for repertoire reconstruction from raw sequencing data. We also provide examples of how immune repertoire profiling can be used to study adaptive immunity in disease and in the course of organ and bone marrow transplantation.

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Section: Clonal Sequence Featuresmentioning

confidence: 99%

T‐cell receptor and B‐cell receptor repertoire profiling in adaptive immunity

2019

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“…A major risk factor specific to SOT is the use of multivisceral or intestinal transplants due to a high volume of donor lymphoid tissue contained in the graft, which is subject to expansion when exposed to EBV and in an immunodeficient environment (Kinch et al , ). Although an intact immune system is essential for chronic viral hepatitis to directly cause a lymphoproliferative disorder, untreated infection with the hepatitis C virus can contribute to PTLD pathogenesis by inducing alterations in the B‐cell receptor immunoglobulin gene and through chronic antigenic stimulation (Morton et al , ; Tucci et al , ). Recipient HLA‐A26 and HLA‐B38 status has also been associated with a higher risk, probably due to altered antigen presentation or immune tolerance (Reshef et al , ).…”

Section: Epidemiologymentioning

confidence: 99%

Management of post‐transplant lymphoproliferative disorders

et al. 2018

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The post-transplant lymphoproliferative disorders (PTLDs) are a heterogeneous group of neoplasms that are one of the most serious complications of bone marrow and solid organ transplants. Because these disorders are rare, there are no randomized trials from which to derive optimal treatment. Management can be challenging and must balance the goal of PTLD eradication with the risks of graft rejection, graft-versus-host disease, further delays in immune reconstitution and life-threatening infections, among others. This paper will provide a comprehensive review of PTLD following solid organ transplant and haematopoietic stem cell transplant with a focus on management. Included is a discussion of novel agents that are being studied in clinical trials and, when combined or sequenced with conventional therapy, have the potential to improve outcomes.

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“…The B cell receptor (BCR), a B cell surface membrane immunoglobulin, possesses the ability to specifically recognize and bind antigens, with the complementarity-determining region 3 (CDR3) of the heavy chain as the major determinant of antibody specificity (Xu and Davis, 2000). The diversity of BCR repertoires in several infectious diseases has been explored, such as in coronavirus disease 2019 (Wen et al, 2020), dengue (Parameswaran et al, 2013), and chronic hepatitis C virus infection (Tucci et al, 2018). These results show that encountering a specific antigen could elicit clonal B-cell proliferation, thus altering the selective distribution of the BCR spectrum.…”

Section: Introductionmentioning

confidence: 99%

Signatures of B Cell Receptor Repertoire Following Pneumocystis Infection

et al. 2021

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B cells play vital roles in host defense against Pneumocystis infection. However, the features of the B cell receptor (BCR) repertoire in disease progression remain unclear. Here, we integrated single-cell RNA sequencing and single-cell BCR sequencing of immune cells from mouse lungs in an uninfected state and 1–4 weeks post-infection in order to illustrate the dynamic nature of B cell responses during Pneumocystis infection. We identified continuously increased plasma cells and an elevated ratio of (IgA + IgG) to (IgD + IgM) after infection. Moreover, Pneumocystis infection was associated with an increasing naïve B subset characterized by elevated expression of the transcription factor ATF3. The proportion of clonal expanded cells progressively increased, while BCR diversity decreased. Plasma cells exhibited higher levels of somatic hypermutation than naïve B cells. Biased usage of V(D)J genes was observed, and the usage frequency of IGHV9-3 rose. Overall, these results present a detailed atlas of B cell transcriptional changes and BCR repertoire features in the context of Pneumocystis infection, which provides valuable information for finding diagnostic biomarkers and developing potential immunotherapeutic targets.

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Biased IGH VDJ gene repertoire and clonal expansions in B cells of chronically hepatitis C virus–infected individuals

Cited by 29 publications

References 51 publications

T‐cell receptor and B‐cell receptor repertoire profiling in adaptive immunity

T‐cell receptor and B‐cell receptor repertoire profiling in adaptive immunity

Management of post‐transplant lymphoproliferative disorders

Signatures of B Cell Receptor Repertoire Following Pneumocystis Infection

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