PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21

Alexandra V. Bocharnikov; Joshua Keegan; Vanessa S. Wacleche; Ye Cao; Chamith Y. Fonseka; Guoxing Wang; Eric S. Muise; Kelvin X. Zhang; Arnon Arazi; Gregory Keras; Zhihan J. Li; Yujie Qu; Michael F. Gurish; Michelle Petri; Jill P. Buyon; Chaim Putterman; David Wofsy; Judith A. James; Joel M. Guthridge; Betty Diamond; Jennifer H. Anolik; Matthew F. Mackey; Stephen E. Alves; Peter A. Nigrovic; Karen H. Costenbader; Michael B. Brenner; James A. Lederer; Deepak A. Rao

doi:10.1172/jci.insight.130062

PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21

Alexandra V. Bocharnikov, Joshua Keegan, Vanessa S. Wacleche, Ye Cao, Chamith Y. Fonseka, Guoxing Wang, Eric S. Muise, Kelvin X. Zhang, Arnon Arazi, Gregory Keras, Zhihan J. Li, Yujie Qu, Michael F. Gurish, Michelle Petri, Jill P. Buyon, Chaim Putterman, David Wofsy, Judith A. James, Joel M. Guthridge, Betty DiamondJennifer H. Anolik, Matthew F. Mackey, Stephen E. Alves, Peter A. Nigrovic, Karen H. Costenbader, Michael B. Brenner, James A. Lederer, Deepak A. Rao

Medicine

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

146 Scopus citations

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by pathologic T cell-B cell interactions and autoantibody production. Defining the T cell populations that drive B cell responses in SLE may enable design of therapies that specifically target pathologic cell subsets. Here, we evaluated the phenotypes of CD4+ T cells in the circulation of 52 SLE patients drawn from multiple cohorts and identified a highly expanded PD-1hiCXCR5-CD4+ T cell population. Cytometric, transcriptomic, and functional assays demonstrated that PD-1hiCXCR5-CD4+ T cells from SLE patients are T peripheral helper (Tph) cells, a CXCR5- T cell population that stimulates B cell responses via IL-21. The frequency of Tph cells, but not T follicular helper (Tfh) cells, correlated with both clinical disease activity and the frequency of CD11c+ B cells in SLE patients. PD-1^hiCD4⁺ T cells were found within lupus nephritis kidneys and correlated with B cell numbers in the kidney. Both IL-21 neutralization and CRISPR-mediated deletion of MAF abrogated the ability of Tph cells to induce memory B cell differentiation into plasmablasts in vitro. These findings identify Tph cells as a highly expanded T cell population in SLE and suggest a key role for Tph cells in stimulating pathologic B cell responses.

Original language	English (US)
Article number	e130062
Journal	JCI Insight
Volume	4
Issue number	20
DOIs	https://doi.org/10.1172/jci.insight.130062
State	Published - Sep 19 2019

ASJC Scopus subject areas

General Medicine

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10.1172/jci.insight.130062

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Bocharnikov, A. V., Keegan, J., Wacleche, V. S., Cao, Y., Fonseka, C. Y., Wang, G., Muise, E. S., Zhang, K. X., Arazi, A., Keras, G., Li, Z. J., Qu, Y., Gurish, M. F., Petri, M., Buyon, J. P., Putterman, C., Wofsy, D., James, J. A., Guthridge, J. M., ... Rao, D. A. (2019). PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21. JCI Insight, 4(20), Article e130062. https://doi.org/10.1172/jci.insight.130062

Bocharnikov, AV, Keegan, J, Wacleche, VS, Cao, Y, Fonseka, CY, Wang, G, Muise, ES, Zhang, KX, Arazi, A, Keras, G, Li, ZJ, Qu, Y, Gurish, MF, Petri, M, Buyon, JP, Putterman, C, Wofsy, D, James, JA, Guthridge, JM, Diamond, B, Anolik, JH, Mackey, MF, Alves, SE, Nigrovic, PA, Costenbader, KH, Brenner, MB, Lederer, JA & Rao, DA 2019, 'PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21', JCI Insight, vol. 4, no. 20, e130062. https://doi.org/10.1172/jci.insight.130062

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title = "PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21",

abstract = "Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by pathologic T cell-B cell interactions and autoantibody production. Defining the T cell populations that drive B cell responses in SLE may enable design of therapies that specifically target pathologic cell subsets. Here, we evaluated the phenotypes of CD4+ T cells in the circulation of 52 SLE patients drawn from multiple cohorts and identified a highly expanded PD-1hiCXCR5-CD4+ T cell population. Cytometric, transcriptomic, and functional assays demonstrated that PD-1hiCXCR5-CD4+ T cells from SLE patients are T peripheral helper (Tph) cells, a CXCR5- T cell population that stimulates B cell responses via IL-21. The frequency of Tph cells, but not T follicular helper (Tfh) cells, correlated with both clinical disease activity and the frequency of CD11c+ B cells in SLE patients. PD-1hiCD4+ T cells were found within lupus nephritis kidneys and correlated with B cell numbers in the kidney. Both IL-21 neutralization and CRISPR-mediated deletion of MAF abrogated the ability of Tph cells to induce memory B cell differentiation into plasmablasts in vitro. These findings identify Tph cells as a highly expanded T cell population in SLE and suggest a key role for Tph cells in stimulating pathologic B cell responses.",

author = "Bocharnikov, {Alexandra V.} and Joshua Keegan and Wacleche, {Vanessa S.} and Ye Cao and Fonseka, {Chamith Y.} and Guoxing Wang and Muise, {Eric S.} and Zhang, {Kelvin X.} and Arnon Arazi and Gregory Keras and Li, {Zhihan J.} and Yujie Qu and Gurish, {Michael F.} and Michelle Petri and Buyon, {Jill P.} and Chaim Putterman and David Wofsy and James, {Judith A.} and Guthridge, {Joel M.} and Betty Diamond and Anolik, {Jennifer H.} and Mackey, {Matthew F.} and Alves, {Stephen E.} and Nigrovic, {Peter A.} and Costenbader, {Karen H.} and Brenner, {Michael B.} and Lederer, {James A.} and Rao, {Deepak A.}",

year = "2019",

month = sep,

day = "19",

doi = "10.1172/jci.insight.130062",

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T1 - PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21

AU - Bocharnikov, Alexandra V.

AU - Keegan, Joshua

AU - Wacleche, Vanessa S.

AU - Cao, Ye

AU - Fonseka, Chamith Y.

AU - Wang, Guoxing

AU - Muise, Eric S.

AU - Zhang, Kelvin X.

AU - Arazi, Arnon

AU - Keras, Gregory

AU - Li, Zhihan J.

AU - Qu, Yujie

AU - Gurish, Michael F.

AU - Petri, Michelle

AU - Buyon, Jill P.

AU - Putterman, Chaim

AU - Wofsy, David

AU - James, Judith A.

AU - Guthridge, Joel M.

AU - Diamond, Betty

AU - Anolik, Jennifer H.

AU - Mackey, Matthew F.

AU - Alves, Stephen E.

AU - Nigrovic, Peter A.

AU - Costenbader, Karen H.

AU - Brenner, Michael B.

AU - Lederer, James A.

AU - Rao, Deepak A.

PY - 2019/9/19

Y1 - 2019/9/19

N2 - Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by pathologic T cell-B cell interactions and autoantibody production. Defining the T cell populations that drive B cell responses in SLE may enable design of therapies that specifically target pathologic cell subsets. Here, we evaluated the phenotypes of CD4+ T cells in the circulation of 52 SLE patients drawn from multiple cohorts and identified a highly expanded PD-1hiCXCR5-CD4+ T cell population. Cytometric, transcriptomic, and functional assays demonstrated that PD-1hiCXCR5-CD4+ T cells from SLE patients are T peripheral helper (Tph) cells, a CXCR5- T cell population that stimulates B cell responses via IL-21. The frequency of Tph cells, but not T follicular helper (Tfh) cells, correlated with both clinical disease activity and the frequency of CD11c+ B cells in SLE patients. PD-1hiCD4+ T cells were found within lupus nephritis kidneys and correlated with B cell numbers in the kidney. Both IL-21 neutralization and CRISPR-mediated deletion of MAF abrogated the ability of Tph cells to induce memory B cell differentiation into plasmablasts in vitro. These findings identify Tph cells as a highly expanded T cell population in SLE and suggest a key role for Tph cells in stimulating pathologic B cell responses.

AB - Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by pathologic T cell-B cell interactions and autoantibody production. Defining the T cell populations that drive B cell responses in SLE may enable design of therapies that specifically target pathologic cell subsets. Here, we evaluated the phenotypes of CD4+ T cells in the circulation of 52 SLE patients drawn from multiple cohorts and identified a highly expanded PD-1hiCXCR5-CD4+ T cell population. Cytometric, transcriptomic, and functional assays demonstrated that PD-1hiCXCR5-CD4+ T cells from SLE patients are T peripheral helper (Tph) cells, a CXCR5- T cell population that stimulates B cell responses via IL-21. The frequency of Tph cells, but not T follicular helper (Tfh) cells, correlated with both clinical disease activity and the frequency of CD11c+ B cells in SLE patients. PD-1hiCD4+ T cells were found within lupus nephritis kidneys and correlated with B cell numbers in the kidney. Both IL-21 neutralization and CRISPR-mediated deletion of MAF abrogated the ability of Tph cells to induce memory B cell differentiation into plasmablasts in vitro. These findings identify Tph cells as a highly expanded T cell population in SLE and suggest a key role for Tph cells in stimulating pathologic B cell responses.

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PD-1hiCXCR5- T peripheral helper cells promote B cell responses in lupus via MAF and IL-21

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