Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis

David Lübbering; Max Preti; Lena Schlott; Christoph Schultheiß; Sören Alexander Weidemann; Ansgar Wilhelm Lohse; Mascha Binder; Antonella Carambia; Johannes Herkel

doi:10.1111/imm.13665

Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis

Standard

Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis. / Lübbering, David; Preti, Max; Schlott, Lena; Schultheiß, Christoph; Weidemann, Sören Alexander ; Lohse, Ansgar Wilhelm; Binder, Mascha; Carambia, Antonella ; Herkel, Johannes.

In: IMMUNOLOGY, Vol. 170, No. 2, 10.2023, p. 214-229.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Lübbering, D, Preti, M, Schlott, L, Schultheiß, C, Weidemann, SA , Lohse, AW, Binder, M, Carambia, A & Herkel, J 2023, 'Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis', IMMUNOLOGY, vol. 170, no. 2, pp. 214-229. https://doi.org/10.1111/imm.13665

APA

Lübbering, D., Preti, M., Schlott, L., Schultheiß, C., Weidemann, S. A., Lohse, A. W., Binder, M., Carambia, A., & Herkel, J. (2023). Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis. IMMUNOLOGY, 170(2), 214-229. https://doi.org/10.1111/imm.13665

Vancouver

Lübbering D, Preti M, Schlott L, Schultheiß C, Weidemann SA , Lohse AW et al. Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis. IMMUNOLOGY. 2023 Oct;170(2):214-229. https://doi.org/10.1111/imm.13665

Bibtex

@article{e6fd2cc6aade4d5c8909cff520e2037a,

title = "Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis",

abstract = "Autoreactive B cells are considered pathogenic drivers in many autoimmune diseases; however, it is not clear whether autoimmune B cells are invariably pathogenic or whether they can also arise as bystanders of T cell-driven autoimmune pathology. Here, we studied the B cell response in an autoantigen- and CD4+ T cell-driven model of autoimmune hepatitis (AIH), the Alb-iGP_Smarta mouse in which expression of a viral model antigen (GP) in hepatocytes and its recognition by GP-specific CD4+ T cells causes spontaneous AIH-like disease. T cell-driven AIH in Alb-iGP_Smarta mice was marked by autoantibodies and hepatic infiltration of plasma cells and B cells, particularly of isotype-switched memory B cells, indicating antigen-driven selection and activation. Immunosequencing of B cell receptor repertoires confirmed B cell expansion selectively in the liver, which was most likely driven by the hepatic GP model antigen, as indicated by branched networks of connected sequences and elevated levels of IgG antibodies to GP. However, intrahepatic B cells did not produce increased levels of cytokines and their depletion with anti-CD20 antibody did not alter the CD4+ T cell response in Alb-iGP_Smarta mice. Moreover, B cell depletion did not prevent spontaneous liver inflammation and AIH-like disease in Alb-iGP_Smarta mice. In conclusion, selection and isotype-switch of liver-infiltrating B cells was dependent on the presence of CD4+ T cells recognizing liver antigen. However, recognition of hepatic antigen by CD4+ T cells and CD4+ T cell-mediated hepatitis was not dependent on B cells. Thus, autoreactive B cells can be bystanders and need not be drivers of liver inflammation in AIH.",

author = "David L{\"u}bbering and Max Preti and Lena Schlott and Christoph Schulthei{\ss} and Weidemann, {S{\"o}ren Alexander} and Lohse, {Ansgar Wilhelm} and Mascha Binder and Antonella Carambia and Johannes Herkel",

year = "2023",

month = oct,

doi = "10.1111/imm.13665",

language = "English",

volume = "170",

pages = "214--229",

journal = "IMMUNOLOGY",

issn = "0019-2805",

publisher = "Wiley-Blackwell",

number = "2",

}

RIS

TY - JOUR

T1 - Autoantigen-selected B cells are bystanders in spontaneous T cell-driven experimental autoimmune hepatitis

AU - Lübbering, David

AU - Preti, Max

AU - Schlott, Lena

AU - Schultheiß, Christoph

AU - Weidemann, Sören Alexander

AU - Lohse, Ansgar Wilhelm

AU - Binder, Mascha

AU - Carambia, Antonella

AU - Herkel, Johannes

PY - 2023/10

Y1 - 2023/10

N2 - Autoreactive B cells are considered pathogenic drivers in many autoimmune diseases; however, it is not clear whether autoimmune B cells are invariably pathogenic or whether they can also arise as bystanders of T cell-driven autoimmune pathology. Here, we studied the B cell response in an autoantigen- and CD4+ T cell-driven model of autoimmune hepatitis (AIH), the Alb-iGP_Smarta mouse in which expression of a viral model antigen (GP) in hepatocytes and its recognition by GP-specific CD4+ T cells causes spontaneous AIH-like disease. T cell-driven AIH in Alb-iGP_Smarta mice was marked by autoantibodies and hepatic infiltration of plasma cells and B cells, particularly of isotype-switched memory B cells, indicating antigen-driven selection and activation. Immunosequencing of B cell receptor repertoires confirmed B cell expansion selectively in the liver, which was most likely driven by the hepatic GP model antigen, as indicated by branched networks of connected sequences and elevated levels of IgG antibodies to GP. However, intrahepatic B cells did not produce increased levels of cytokines and their depletion with anti-CD20 antibody did not alter the CD4+ T cell response in Alb-iGP_Smarta mice. Moreover, B cell depletion did not prevent spontaneous liver inflammation and AIH-like disease in Alb-iGP_Smarta mice. In conclusion, selection and isotype-switch of liver-infiltrating B cells was dependent on the presence of CD4+ T cells recognizing liver antigen. However, recognition of hepatic antigen by CD4+ T cells and CD4+ T cell-mediated hepatitis was not dependent on B cells. Thus, autoreactive B cells can be bystanders and need not be drivers of liver inflammation in AIH.

AB - Autoreactive B cells are considered pathogenic drivers in many autoimmune diseases; however, it is not clear whether autoimmune B cells are invariably pathogenic or whether they can also arise as bystanders of T cell-driven autoimmune pathology. Here, we studied the B cell response in an autoantigen- and CD4+ T cell-driven model of autoimmune hepatitis (AIH), the Alb-iGP_Smarta mouse in which expression of a viral model antigen (GP) in hepatocytes and its recognition by GP-specific CD4+ T cells causes spontaneous AIH-like disease. T cell-driven AIH in Alb-iGP_Smarta mice was marked by autoantibodies and hepatic infiltration of plasma cells and B cells, particularly of isotype-switched memory B cells, indicating antigen-driven selection and activation. Immunosequencing of B cell receptor repertoires confirmed B cell expansion selectively in the liver, which was most likely driven by the hepatic GP model antigen, as indicated by branched networks of connected sequences and elevated levels of IgG antibodies to GP. However, intrahepatic B cells did not produce increased levels of cytokines and their depletion with anti-CD20 antibody did not alter the CD4+ T cell response in Alb-iGP_Smarta mice. Moreover, B cell depletion did not prevent spontaneous liver inflammation and AIH-like disease in Alb-iGP_Smarta mice. In conclusion, selection and isotype-switch of liver-infiltrating B cells was dependent on the presence of CD4+ T cells recognizing liver antigen. However, recognition of hepatic antigen by CD4+ T cells and CD4+ T cell-mediated hepatitis was not dependent on B cells. Thus, autoreactive B cells can be bystanders and need not be drivers of liver inflammation in AIH.

U2 - 10.1111/imm.13665

DO - 10.1111/imm.13665

M3 - SCORING: Journal article

C2 - 37243425

VL - 170

SP - 214

EP - 229

JO - IMMUNOLOGY

JF - IMMUNOLOGY

SN - 0019-2805

IS - 2

ER -