Influence of Fas on the regulation of the response of an anti-nuclear antigen B cell clonotype to foreign antigen

doi:10.1093/intimm/dxn087

International Immunology Advance Access originally published online on August 8, 2008
International Immunology 2008 20(10):1279-1287; doi:10.1093/intimm/dxn087

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Influence of Fas on the regulation of the response of an anti-nuclear antigen B cell clonotype to foreign antigen

Boris Alabyev¹^,2, Raja Vuyyuru¹ and Tim Manser¹

¹ Department of Microbiology and Immunology, Thomas Jefferson University, Jefferson Alumni Hall 471, 1020 Locust Street, Philadelphia, PA 19107, USA
² Present address: Department of Pathology, University of Maryland Medical School, Baltimore, MD, USA

Correspondence to: T. Manser; E-mail: manser{at}mail.jci.tju.edu

A peripheral B cell tolerance checkpoint appears to be operativeduring the germinal center (GC) reaction. We previously showedthat a transgenic BCR clonotype that is ‘dual reactive’for the hapten arsonate (Ars) and nuclear auto-antigens is stimulatedto enter the GC response via Ars immunization. However, theparticipation of this clonotype in this response wanes withtime and it gives rise to few memory B cells capable of mountinga secondary anti-Ars IgG response. Enforced expression of Bcl-2partially rescues the GC and memory B cell responses of thisclonotype, suggesting that apoptotic pathways are involved inthe action of the GC tolerance checkpoint. Since GC B cellssubstantially up-regulate levels of expression of the Fas apoptoticdeath receptor, we determined whether an intrinsic Fas deficientcould rescue the participation of this clonotype in the GC response.It could not, strongly indicating that Fas expression by autoreactiveGC B cells is not necessary for their elimination. In addition,experiments in which Fas-sufficient dual reactive clonotypeB cells were transferred to Fas-deficient hosts revealed anabsence of participation of these B cells in the GC and IgGanti-Ars responses. We present data consistent with the ideathat T cells in Fas-deficient hosts are primed to express elevatedlevels of FasL and eliminate antigen-activated B cells thatup-regulate Fas.

Keywords: B cell, Fas death receptor, Fas ligand, germinal center, tolerance

Transmitting editor: J. Ravetch

Received 10 March 2008, accepted 1 July 2008.

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