Aberrant zonal recycling of germinal center B cells impairs appropriate selection in lupus

Gina M. Sanchez; Eden S. Hirsch; Arthur VanValkenburg; Daniel P. Mayer; Komi Gbedande; Rebecca L. Francis; Wenzhi Song; Olivia Q. Antao; Kyleigh E. Brimmer; Alexander Lemenze; Robin Stephens; W. Evan Johnson; Jason S. Weinstein

doi:10.1016/j.celrep.2024.114978

Aberrant zonal recycling of germinal center B cells impairs appropriate selection in lupus

Gina M. Sanchez, Eden S. Hirsch, Arthur VanValkenburg, Daniel P. Mayer, Komi Gbedande, Rebecca L. Francis, Wenzhi Song, Olivia Q. Antao, Kyleigh E. Brimmer, Alexander Lemenze, Robin Stephens, W. Evan Johnson, Jason S. Weinstein

Research output: Contribution to journal › Article › peer-review

Abstract

Autoimmune diseases such as lupus are characterized by polyclonal B cell activation, leading to the production of autoantibodies. The mechanism leading to B cell dysregulation is unclear; however, the defect may lie in selection within germinal centers (GCs). GC B cells cycle between proliferation and mutation in the dark zone and selection in the light zone (LZ). Temporal assessment of GCs from mice with either persistent infection or lupus showed an accumulation of LZ B cells. Yet, only in lupus, GC B cells exhibited reduced proliferation and progressive loss of MYC and FOXO1, which regulate zonal recycling and differentiation. As lupus progressed, decreased mutational frequency and repertoire diversity were associated with reduced responsiveness to CD40 signaling, despite accumulation of plasma cells. Collectively, these findings suggest that lupus disease progression coincides with an intrinsic defect in LZ B cell signaling, altering the zonal recycling, selection, and differentiation of autoreactive B cells.

Original language	English (US)
Article number	114978
Journal	Cell Reports
Volume	43
Issue number	11
DOIs	https://doi.org/10.1016/j.celrep.2024.114978
State	Published - Nov 26 2024

All Science Journal Classification (ASJC) codes

General Biochemistry, Genetics and Molecular Biology

Keywords

B cells
CP: Immunology
autoimmunity
germinal center

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10.1016/j.celrep.2024.114978

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Sanchez, G. M., Hirsch, E. S., VanValkenburg, A., Mayer, D. P., Gbedande, K., Francis, R. L., Song, W., Antao, O. Q., Brimmer, K. E., Lemenze, A., Stephens, R., Johnson, W. E., & Weinstein, J. S. (2024). Aberrant zonal recycling of germinal center B cells impairs appropriate selection in lupus. Cell Reports, 43(11), Article 114978. https://doi.org/10.1016/j.celrep.2024.114978

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title = "Aberrant zonal recycling of germinal center B cells impairs appropriate selection in lupus",

abstract = "Autoimmune diseases such as lupus are characterized by polyclonal B cell activation, leading to the production of autoantibodies. The mechanism leading to B cell dysregulation is unclear; however, the defect may lie in selection within germinal centers (GCs). GC B cells cycle between proliferation and mutation in the dark zone and selection in the light zone (LZ). Temporal assessment of GCs from mice with either persistent infection or lupus showed an accumulation of LZ B cells. Yet, only in lupus, GC B cells exhibited reduced proliferation and progressive loss of MYC and FOXO1, which regulate zonal recycling and differentiation. As lupus progressed, decreased mutational frequency and repertoire diversity were associated with reduced responsiveness to CD40 signaling, despite accumulation of plasma cells. Collectively, these findings suggest that lupus disease progression coincides with an intrinsic defect in LZ B cell signaling, altering the zonal recycling, selection, and differentiation of autoreactive B cells.",

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author = "Sanchez, {Gina M.} and Hirsch, {Eden S.} and Arthur VanValkenburg and Mayer, {Daniel P.} and Komi Gbedande and Francis, {Rebecca L.} and Wenzhi Song and Antao, {Olivia Q.} and Brimmer, {Kyleigh E.} and Alexander Lemenze and Robin Stephens and Johnson, {W. Evan} and Weinstein, {Jason S.}",

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year = "2024",

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doi = "10.1016/j.celrep.2024.114978",

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AU - Sanchez, Gina M.

AU - Hirsch, Eden S.

AU - VanValkenburg, Arthur

AU - Mayer, Daniel P.

AU - Gbedande, Komi

AU - Francis, Rebecca L.

AU - Song, Wenzhi

AU - Antao, Olivia Q.

AU - Brimmer, Kyleigh E.

AU - Lemenze, Alexander

AU - Stephens, Robin

AU - Johnson, W. Evan

AU - Weinstein, Jason S.

PY - 2024/11/26

Y1 - 2024/11/26

N2 - Autoimmune diseases such as lupus are characterized by polyclonal B cell activation, leading to the production of autoantibodies. The mechanism leading to B cell dysregulation is unclear; however, the defect may lie in selection within germinal centers (GCs). GC B cells cycle between proliferation and mutation in the dark zone and selection in the light zone (LZ). Temporal assessment of GCs from mice with either persistent infection or lupus showed an accumulation of LZ B cells. Yet, only in lupus, GC B cells exhibited reduced proliferation and progressive loss of MYC and FOXO1, which regulate zonal recycling and differentiation. As lupus progressed, decreased mutational frequency and repertoire diversity were associated with reduced responsiveness to CD40 signaling, despite accumulation of plasma cells. Collectively, these findings suggest that lupus disease progression coincides with an intrinsic defect in LZ B cell signaling, altering the zonal recycling, selection, and differentiation of autoreactive B cells.

AB - Autoimmune diseases such as lupus are characterized by polyclonal B cell activation, leading to the production of autoantibodies. The mechanism leading to B cell dysregulation is unclear; however, the defect may lie in selection within germinal centers (GCs). GC B cells cycle between proliferation and mutation in the dark zone and selection in the light zone (LZ). Temporal assessment of GCs from mice with either persistent infection or lupus showed an accumulation of LZ B cells. Yet, only in lupus, GC B cells exhibited reduced proliferation and progressive loss of MYC and FOXO1, which regulate zonal recycling and differentiation. As lupus progressed, decreased mutational frequency and repertoire diversity were associated with reduced responsiveness to CD40 signaling, despite accumulation of plasma cells. Collectively, these findings suggest that lupus disease progression coincides with an intrinsic defect in LZ B cell signaling, altering the zonal recycling, selection, and differentiation of autoreactive B cells.

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Aberrant zonal recycling of germinal center B cells impairs appropriate selection in lupus

Abstract

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