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The Journal of Immunology, 2007, 178: 93.22.
Copyright © 2007 by The American Association of Immunologists, Inc.

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93.22

Partial MHC Class II molecules preferentially bind to B cells

Jason M Link1, Roberto Meza-Romero2, Michael Afentoulis1, Marisa Agotsch2, Dorian LaTocha1, Gregory Burrows2 and Arthur A Vandenbark1,2

1 Portland Veterans Affairs Medical Center, 3710 SW U.S. Veterans Hospital Road, Portland, OR, 97239, 2 Neurology, Oregon Health & Science University, 3181 S.W. Sam Jackson Park Rd., Portland, OR, 97239

Abstract

Recombinant, two-domain MHC Class II proteins ({alpha}1beta1MHCII) that lack sequence from the membrane proximal {alpha}2 and beta2 domains of MHC Class II adhere preferentially to B cells in vivo and ex vivo; whereas, full length (four-domain) constructs do not bind. Because {alpha}1beta1MHCII molecules that contain only native MHC Class II sequence have preferential affinity for B cells, we hypothesize that a natural, cell-free form of MHC Class II (similar to recombinant {alpha}1beta1MHCII) exists and has affinity for a receptor expressed by B cells. Evidence that endogenous, natural MHC Class II molecules transfer to B cells and that {alpha}1beta1MHCII has inter- and intra-species affinity for B cells suggest that this is a natural and evolutionarily conserved property. And evidence that {alpha}1beta1MHCII can stimulate CD4+ T cells suggests that there is an immune function for partial, cell-free MHC Class II. Transfer of immunoreactive, cell-free {alpha}1beta1MHCII/Ag complexes to B cells suggests a here-to-fore unrecognized pathway for T cell activation.





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