Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.

Alexandre Belot; Paul R Kasher; Eleanor W Trotter; Anne-Perrine Foray; Anne-Laure Debaud; Gillian I Rice; Marcin Szynkiewicz; Marie-Therese Zabot; Isabelle Rouvet; Sanjeev S Bhaskar; Sarah B Daly; Jonathan E Dickerson; Josephine Mayer; James O'Sullivan; Laurent Juillard; Jill E Urquhart; Shameem Fawdar; Anna A Marusiak; Natalie Stephenson; Bohdan Waszkowycz; Michael W Beresford; Leslie G Biesecker; Graeme C M Black; Céline René; Jean-François Eliaou; Nicole Fabien; Bruno Ranchin; Pierre Cochat; Patrick M Gaffney; Flore Rozenberg; Pierre Lebon; Christophe Malcus; Yanick J Crow; John Brognard; Nathalie Bonnefoy

doi:10.1002/art.38008

Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.

Alexandre Belot, Paul R Kasher, Eleanor W Trotter, Anne-Perrine Foray, Anne-Laure Debaud, Gillian I Rice, Marcin Szynkiewicz, Marie-Therese Zabot, Isabelle Rouvet, Sanjeev S Bhaskar, Sarah B Daly, Jonathan E Dickerson, Josephine Mayer, James O'Sullivan, Laurent Juillard, Jill E Urquhart, Shameem Fawdar, Anna A Marusiak, Natalie Stephenson, Bohdan WaszkowyczMichael W Beresford, Leslie G Biesecker, Graeme C M Black, Céline René, Jean-François Eliaou, Nicole Fabien, Bruno Ranchin, Pierre Cochat, Patrick M Gaffney, Flore Rozenberg, Pierre Lebon, Christophe Malcus, Yanick J Crow, John Brognard, Nathalie Bonnefoy

Cancer Research UK Manchester Institute

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

Abstract

OBJECTIVE: Systemic lupus erythematosus (SLE) is a prototype autoimmune disease that is assumed to occur via a complex interplay of environmental and genetic factors. Rare causes of monogenic SLE have been described, providing unique insights into fundamental mechanisms of immune tolerance. The aim of this study was to identify the cause of an autosomal-recessive form of SLE. METHODS: We studied 3 siblings with juvenile-onset SLE from 1 consanguineous kindred and used next-generation sequencing to identify mutations in the disease-associated gene. We performed extensive biochemical, immunologic, and functional assays to assess the impact of the identified mutations on B cell biology. RESULTS: We identified a homozygous missense mutation in PRKCD, encoding protein kinase δ (PKCδ), in all 3 affected siblings. Mutation of PRKCD resulted in reduced expression and activity of the encoded protein PKCδ (involved in the deletion of autoreactive B cells), leading to resistance to B cell receptor- and calcium-dependent apoptosis and increased B cell proliferation. Thus, as for mice deficient in PKCδ, which exhibit an SLE phenotype and B cell expansion, we observed an increased number of immature B cells in the affected family members and a developmental shift toward naive B cells with an immature phenotype. CONCLUSION: Our findings indicate that PKCδ is crucial in regulating B cell tolerance and preventing self-reactivity in humans, and that PKCδ deficiency represents a novel genetic defect of apoptosis leading to SLE.

Original language	English
Pages (from-to)	2161-2171
Number of pages	10
Journal	Arthritis Care & Research
Volume	65
Issue number	8
DOIs	https://doi.org/10.1002/art.38008
Publication status	Published - Aug 2013

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Belot, A., Kasher, P. R., Trotter, E. W., Foray, A.-P., Debaud, A.-L., Rice, G. I., Szynkiewicz, M., Zabot, M.-T., Rouvet, I., Bhaskar, S. S., Daly, S. B., Dickerson, J. E., Mayer, J., O'Sullivan, J., Juillard, L., Urquhart, J. E., Fawdar, S., Marusiak, A. A., Stephenson, N., ... Bonnefoy, N. (2013). Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation. Arthritis Care & Research, 65(8), 2161-2171. https://doi.org/10.1002/art.38008

@article{de42a443c8cf4dcaba0a5c6d79007aa4,

title = "Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.",

abstract = "OBJECTIVE: Systemic lupus erythematosus (SLE) is a prototype autoimmune disease that is assumed to occur via a complex interplay of environmental and genetic factors. Rare causes of monogenic SLE have been described, providing unique insights into fundamental mechanisms of immune tolerance. The aim of this study was to identify the cause of an autosomal-recessive form of SLE. METHODS: We studied 3 siblings with juvenile-onset SLE from 1 consanguineous kindred and used next-generation sequencing to identify mutations in the disease-associated gene. We performed extensive biochemical, immunologic, and functional assays to assess the impact of the identified mutations on B cell biology. RESULTS: We identified a homozygous missense mutation in PRKCD, encoding protein kinase δ (PKCδ), in all 3 affected siblings. Mutation of PRKCD resulted in reduced expression and activity of the encoded protein PKCδ (involved in the deletion of autoreactive B cells), leading to resistance to B cell receptor- and calcium-dependent apoptosis and increased B cell proliferation. Thus, as for mice deficient in PKCδ, which exhibit an SLE phenotype and B cell expansion, we observed an increased number of immature B cells in the affected family members and a developmental shift toward naive B cells with an immature phenotype. CONCLUSION: Our findings indicate that PKCδ is crucial in regulating B cell tolerance and preventing self-reactivity in humans, and that PKCδ deficiency represents a novel genetic defect of apoptosis leading to SLE.",

author = "Alexandre Belot and Kasher, {Paul R} and Trotter, {Eleanor W} and Anne-Perrine Foray and Anne-Laure Debaud and Rice, {Gillian I} and Marcin Szynkiewicz and Marie-Therese Zabot and Isabelle Rouvet and Bhaskar, {Sanjeev S} and Daly, {Sarah B} and Dickerson, {Jonathan E} and Josephine Mayer and James O'Sullivan and Laurent Juillard and Urquhart, {Jill E} and Shameem Fawdar and Marusiak, {Anna A} and Natalie Stephenson and Bohdan Waszkowycz and {W Beresford}, Michael and Biesecker, {Leslie G} and {C M Black}, Graeme and C{\'e}line Ren{\'e} and Jean-Fran{\c c}ois Eliaou and Nicole Fabien and Bruno Ranchin and Pierre Cochat and Gaffney, {Patrick M} and Flore Rozenberg and Pierre Lebon and Christophe Malcus and Crow, {Yanick J} and John Brognard and Nathalie Bonnefoy",

note = "C5759/A12328, Cancer Research UK, United KingdomR01 AI063274, NIAID NIH HHS, United StatesR01-AI-063274, NIAID NIH HHS, United StatesRC2 AR058959, NIAMS NIH HHS, United StatesRC2-AR-058959, NIAMS NIH HHS, United States",

year = "2013",

month = aug,

doi = "10.1002/art.38008",

language = "English",

volume = "65",

pages = "2161--2171",

journal = "Arthritis Care & Research",

issn = "2151-4658",

publisher = "John Wiley & Sons Ltd",

number = "8",

}

Belot, A, Kasher, PR, Trotter, EW, Foray, A-P, Debaud, A-L, Rice, GI, Szynkiewicz, M, Zabot, M-T, Rouvet, I, Bhaskar, SS, Daly, SB, Dickerson, JE, Mayer, J, O'Sullivan, J, Juillard, L, Urquhart, JE, Fawdar, S, Marusiak, AA, Stephenson, N, Waszkowycz, B, W Beresford, M, Biesecker, LG, C M Black, G, René, C, Eliaou, J-F, Fabien, N, Ranchin, B, Cochat, P, Gaffney, PM, Rozenberg, F, Lebon, P, Malcus, C, Crow, YJ, Brognard, J & Bonnefoy, N 2013, 'Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.', Arthritis Care & Research, vol. 65, no. 8, pp. 2161-2171. https://doi.org/10.1002/art.38008

TY - JOUR

T1 - Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.

AU - Belot, Alexandre

AU - Kasher, Paul R

AU - Trotter, Eleanor W

AU - Foray, Anne-Perrine

AU - Debaud, Anne-Laure

AU - Rice, Gillian I

AU - Szynkiewicz, Marcin

AU - Zabot, Marie-Therese

AU - Rouvet, Isabelle

AU - Bhaskar, Sanjeev S

AU - Daly, Sarah B

AU - Dickerson, Jonathan E

AU - Mayer, Josephine

AU - O'Sullivan, James

AU - Juillard, Laurent

AU - Urquhart, Jill E

AU - Fawdar, Shameem

AU - Marusiak, Anna A

AU - Stephenson, Natalie

AU - Waszkowycz, Bohdan

AU - W Beresford, Michael

AU - Biesecker, Leslie G

AU - C M Black, Graeme

AU - René, Céline

AU - Eliaou, Jean-François

AU - Fabien, Nicole

AU - Ranchin, Bruno

AU - Cochat, Pierre

AU - Gaffney, Patrick M

AU - Rozenberg, Flore

AU - Lebon, Pierre

AU - Malcus, Christophe

AU - Crow, Yanick J

AU - Brognard, John

AU - Bonnefoy, Nathalie

N1 - C5759/A12328, Cancer Research UK, United KingdomR01 AI063274, NIAID NIH HHS, United StatesR01-AI-063274, NIAID NIH HHS, United StatesRC2 AR058959, NIAMS NIH HHS, United StatesRC2-AR-058959, NIAMS NIH HHS, United States

PY - 2013/8

Y1 - 2013/8

N2 - OBJECTIVE: Systemic lupus erythematosus (SLE) is a prototype autoimmune disease that is assumed to occur via a complex interplay of environmental and genetic factors. Rare causes of monogenic SLE have been described, providing unique insights into fundamental mechanisms of immune tolerance. The aim of this study was to identify the cause of an autosomal-recessive form of SLE. METHODS: We studied 3 siblings with juvenile-onset SLE from 1 consanguineous kindred and used next-generation sequencing to identify mutations in the disease-associated gene. We performed extensive biochemical, immunologic, and functional assays to assess the impact of the identified mutations on B cell biology. RESULTS: We identified a homozygous missense mutation in PRKCD, encoding protein kinase δ (PKCδ), in all 3 affected siblings. Mutation of PRKCD resulted in reduced expression and activity of the encoded protein PKCδ (involved in the deletion of autoreactive B cells), leading to resistance to B cell receptor- and calcium-dependent apoptosis and increased B cell proliferation. Thus, as for mice deficient in PKCδ, which exhibit an SLE phenotype and B cell expansion, we observed an increased number of immature B cells in the affected family members and a developmental shift toward naive B cells with an immature phenotype. CONCLUSION: Our findings indicate that PKCδ is crucial in regulating B cell tolerance and preventing self-reactivity in humans, and that PKCδ deficiency represents a novel genetic defect of apoptosis leading to SLE.

AB - OBJECTIVE: Systemic lupus erythematosus (SLE) is a prototype autoimmune disease that is assumed to occur via a complex interplay of environmental and genetic factors. Rare causes of monogenic SLE have been described, providing unique insights into fundamental mechanisms of immune tolerance. The aim of this study was to identify the cause of an autosomal-recessive form of SLE. METHODS: We studied 3 siblings with juvenile-onset SLE from 1 consanguineous kindred and used next-generation sequencing to identify mutations in the disease-associated gene. We performed extensive biochemical, immunologic, and functional assays to assess the impact of the identified mutations on B cell biology. RESULTS: We identified a homozygous missense mutation in PRKCD, encoding protein kinase δ (PKCδ), in all 3 affected siblings. Mutation of PRKCD resulted in reduced expression and activity of the encoded protein PKCδ (involved in the deletion of autoreactive B cells), leading to resistance to B cell receptor- and calcium-dependent apoptosis and increased B cell proliferation. Thus, as for mice deficient in PKCδ, which exhibit an SLE phenotype and B cell expansion, we observed an increased number of immature B cells in the affected family members and a developmental shift toward naive B cells with an immature phenotype. CONCLUSION: Our findings indicate that PKCδ is crucial in regulating B cell tolerance and preventing self-reactivity in humans, and that PKCδ deficiency represents a novel genetic defect of apoptosis leading to SLE.

U2 - 10.1002/art.38008

DO - 10.1002/art.38008

M3 - Article

C2 - 23666743

SN - 2151-4658

VL - 65

SP - 2161

EP - 2171

JO - Arthritis Care & Research

JF - Arthritis Care & Research

IS - 8

ER -

Protein kinase cδ deficiency causes mendelian systemic lupus erythematosus with B cell-defective apoptosis and hyperproliferation.

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