Genetic ablation of the Lyn tyrosine kinase has revealed unique inhibitory roles in B lymphocyte signaling. We now report the consequences of sustained activation of Lyn in vivo using a targeted gain-of-function mutation (Lynup/up mice). Lynup/up mice have reduced numbers of conventional B lymphocytes, down-regulated surface immunoglobulin M and costimulatory molecules, and elevated numbers of B1a B cells. Lynup/up B cells are characterized by the constitutive phosphorylation of negative regulators of B cell antigen receptor (BCR) signaling including CD22, SHP-1, and SHIP-1, and display attributes of lymphocytes rendered tolerant by constitutive engagement of the antigen receptor. However, exaggerated positive signaling is also apparent as evidenced by the constitutive phosphorylation of Syk and phospholipase Cγ2 in resting Lynup/up B cells. Similarly, Lynup/up B cells show a heightened calcium flux in response to BCR stimulation. Surprisingly, Lynup/up mice develop circulating autoreactive antibodies and lethal autoimmune glomerulonephritis, suggesting that enhanced positive signaling eventually overrides constitutive negative signaling. These studies highlight the difficulty in maintaining tolerance in the face of chronic stimulation and emphasize the pivotal role of Lyn in B cell signaling.
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16 December 2002
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December 16 2002
Sustained Activation of Lyn Tyrosine Kinase In Vivo Leads to Autoimmunity
Margaret L. Hibbs,
Margaret L. Hibbs
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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Kenneth W. Harder,
Kenneth W. Harder
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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Jane Armes,
Jane Armes
3Melbourne Pathology, Royal Women's Hospital, Victoria 3053, Australia and Victorian Breast Cancer Research Consortium, Department of Pathology, University of Melbourne, Victoria 3052, Australia
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Nicole Kountouri,
Nicole Kountouri
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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Cathy Quilici,
Cathy Quilici
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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Franca Casagranda,
Franca Casagranda
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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Ashley R. Dunn,
Ashley R. Dunn
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
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David M. Tarlinton
David M. Tarlinton
2Walter and Eliza Hall Institute of Medical Research, Royal Melbourne Hospital, Victoria 3050, Australia
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Margaret L. Hibbs
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
Kenneth W. Harder
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
Jane Armes
3Melbourne Pathology, Royal Women's Hospital, Victoria 3053, Australia and Victorian Breast Cancer Research Consortium, Department of Pathology, University of Melbourne, Victoria 3052, Australia
Nicole Kountouri
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
Cathy Quilici
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
Franca Casagranda
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
Ashley R. Dunn
1Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch
David M. Tarlinton
2Walter and Eliza Hall Institute of Medical Research, Royal Melbourne Hospital, Victoria 3050, Australia
Address correspondence to Margaret L. Hibbs, Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch, P.O. Box 2008, Royal Melbourne Hospital, Victoria 3050, Australia. Phone: 61-3-9341-3155; Fax: 61-3-9341-319; E-mail: [email protected]
*
Abbreviations used in this paper: BCR, B cell antigen receptor; BM, bone marrow; BrdU, 5-bromo-2′ deoxyuridine; [Ca2+]i, intracellular calcium concentration; HEL, hen egg lysozyme; HRP, horseradish peroxidase; PLCγ2, phospholipase Cγ2; PY, phosphotyrosine.
Received:
April 02 2002
Revision Received:
November 01 2002
Accepted:
November 04 2002
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2002
J Exp Med (2002) 196 (12): 1593–1604.
Article history
Received:
April 02 2002
Revision Received:
November 01 2002
Accepted:
November 04 2002
Citation
Margaret L. Hibbs, Kenneth W. Harder, Jane Armes, Nicole Kountouri, Cathy Quilici, Franca Casagranda, Ashley R. Dunn, David M. Tarlinton; Sustained Activation of Lyn Tyrosine Kinase In Vivo Leads to Autoimmunity . J Exp Med 16 December 2002; 196 (12): 1593–1604. doi: https://doi.org/10.1084/jem.20020515
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