Hepatitis C viraemia reversibly maintains subset of antigen‐specific T‐bet+ tissue‐like memory B cells

Chang, Li-Yuan; Li, Y.; Kaplan, David E.

doi:10.1111/jvh.12659

Cited by 77 publications

(78 citation statements)

References 27 publications

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“…We also observed involvement of T-bet + B cells in the response to HIV infection, as T-bet was rapidly induced in B cells during the acute phase and T-bet We and others have previously demonstrated an expansion of CD21 -B cell subsets induced by Th1-type human infections, including HIV, malaria, and hepatitis C (30,31,34,35,(60)(61)(62)(63), and expansion of a clonal CD21 -subset has been described during hepatitis B-and hepatitis C-associated mixed cryoglobulinemia (64)(65)(66). Interestingly, maintenance of expanded CD21 -cells in each of these infections appears to be dependent upon pathogen load (34,35,60,(67)(68)(69).…”

Section: Discussionmentioning

confidence: 86%

“…Similarly, chronic lymphochoriomeningitis (LCMV) viremia is controlled to low levels only in the presence of T-bet + B cells via a chiefly IgG2a-dependent mechanism (6). We previously identified a subset of T-bet-expressing B cells in healthy human blood (26), and B cells expressing either TBX21 transcript or T-bet protein have been described in the context of autoimmune disease, chronic hepatitis C infection, and malaria infection (27)(28)(29)(30)(31), but the biological niche of this population in humans has not been defined.…”

Section: Introductionmentioning

confidence: 99%

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T-bet+ B cells are induced by human viral infections and dominate the HIV gp140 response

et al. 2017

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Section: Discussionmentioning

confidence: 86%

Section: Introductionmentioning

confidence: 99%

T-bet+ B cells are induced by human viral infections and dominate the HIV gp140 response

et al. 2017

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“…We found that only memory B cells express SASP markers, especially the terminally differentiated B cell subset (CD19+IgD− CD27−), called late-memory/exhausted-memory, tissuelike, or double negative, which of all B cell subsets is the most pro-inflammatory. This subset has been reported to be increased in the blood of healthy elderly individuals 85,90 and in patients with autoimmune 96–101 and infectious diseases, 102–104 suggesting that, in a favorable inflammatory microenvironment, these cells may expand in vivo in the presence of autoantigens or pathogen-derived antigens, leading to the production of pathogenic (autoimmune) or protective antibodies, respectively.…”

Section: Predictors Of Optimal Vaccine Responsesmentioning

confidence: 99%

B Cell–Specific Biomarkers for Optimal Antibody Responses to Influenza Vaccination and Molecular Pathways That Reduce B Cell Function with Aging

Frasca

Blomberg

2016

Crit Rev Immunol

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This review highlights recent findings on the effects of aging on influenza vaccine responses, with major emphasis on T and B cells, which are significantly impaired by aging. We discuss changes in T cell production and thymic output; T cell subsets; and TCR repertoire, function, and response to latent persistent infection. We also discuss changes in B cell subsets, repertoire, and function, and how function is impaired by increased intrinsic B cell inflammation and reduced signal transduction. This review presents age-related effects on antigen-presenting cells, summarizes recent studies, including our own, aimed at the identification of biomarkers of protective vaccine responses, and provides examples of recent technical advances and insights into human vaccine responses that are helping to define the features associated with successful vaccination and that may enable a more predictive vaccinology in the future.

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“…Recent data suggest that the T-box expressed in T cells (T-bet) transcription factor, critical for inducing sterilizing humoral immunity in acute infections, 6 may also regulate the exhausted state in both autoreactive 7 and antigeninduced anergic B cells. 8,9 No data to date specifically link the anergy properties observed in cryoglobulin-producing B cells and T-bet, but there are phenotypic similarities (CD11c 1 /CD21 low ) that suggest a possible relationship that should be explored; rapid upregulation of T-bet in convalescent CD21 low B cells upon reexposure to autologous HCV strains ex vivo has been observed, 8 suggesting a link between B-cell receptor ligation, T-bet, and the CD21 low exhaustion phenotype.…”

mentioning

confidence: 99%

“…ixed cryoglobulinemia is one of several B-cell proliferative disorders that may result from chronic hepatitis C infection, and it is thought to be driven by expansion of HCV envelope-specific B cells that preferentially use immunoglobulin gene segments V H 1-69 and V k [3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20]3 and to evolve rheumatoid factor activity through somatic hypermutation.…”

mentioning

confidence: 99%

Persistence of exhaustion in cured hep C

Kaplan

2017

Blood

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In this issue of Blood, Del Padre et al 1 evaluated the impact of eliminating chronic antigen exposure on B-cell exhaustion in the human therapeutic setting of directacting antiviral therapy for chronic hepatitis C virus infection (HCV) complicated by mixed cryoglobulinemia (MC). The phenotype of hepatitis C-related MC B cells has been previously demonstrated by this group and others 2 to include low-level CD21 expression (CD21 low ) and hypoproliferation in response to stimulation either through the B-cell receptor or Toll-like receptor 9, imperfectly termed "exhausted" or "anergic." At baseline, CD21 low B cells from HCVinfected patients expressed markers of chronic activation, with elevated and nearmaximal basal levels of phosphorylated extracellular signal-regulated kinase, and were also predisposed to apoptosis. During oral direct-acting antiviral therapy, the authors observed that by 4 weeks (at which point, most patients have no circulating HCV RNA), these basal abnormalities at least partially normalized. During longitudinal follow-up after patients were documented as cured, the overall frequency of CD21 low cells progressively declined from 50% to 30% of circulating B cells. However, the frequency of V H 1-69 1 B cells specific for HCVrelated MC generally remained stable, although some regained CD21 expression. Despite partial resolution of the exhaustion phenotype, surviving V H 1-69 1 B cells remained hypoproliferative upon Toll-like receptor 9 ligation, suggesting that the B-cell exhaustion phenotype is durably programmed into antigen-specific B cells during long-term extracellular antigen exposure. Mixed cryoglobulinemia is one of several B-cell proliferative disorders that may result from chronic hepatitis C infection, and it is thought to be driven by expansion of HCV envelope-specific B cells that preferentially use immunoglobulin gene segments V H 1-69 and V k [3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20]3 and to evolve rheumatoid factor activity through somatic hypermutation. 4Although MC is an infrequent complication of chronic hepatitis C infection, the technological ability to identify and isolate HCV-specific B cells via an anti-idiotype V H 1-69-specific antibody (G6) has made this condition an important model for studying humoral immune dysfunction during human chronic viral infection. Prior studies have identified that V H 1-69 1 B cells manifest genetic signatures of enhanced interferon-mediated responsiveness, apoptosis, and B-cell anergy; are phenotypically most commonly CD27

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Hepatitis C viraemia reversibly maintains subset of antigen‐specific T‐bet+ tissue‐like memory B cells

Cited by 77 publications

References 27 publications

T-bet+ B cells are induced by human viral infections and dominate the HIV gp140 response

T-bet+ B cells are induced by human viral infections and dominate the HIV gp140 response

B Cell–Specific Biomarkers for Optimal Antibody Responses to Influenza Vaccination and Molecular Pathways That Reduce B Cell Function with Aging

Persistence of exhaustion in cured hep C

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