CD5 is a 67-kD glycoprotein that is expressed on most T lymphocytes and on a subset of mature B cells. Although its physiologic function is unknown, several lines of evidence suggest that CD5 may play a role in the regulation of T cell activation and in T cell-antigen presenting cell interactions. Using a CD5-immunoglobulin fusion protein (CD5Rg, for receptorglobulin) we have uncovered a new CD5 ligand (CD5L) expressed on the surface of activated splenocytes. Stimulation of murine splenocytes with anti-CD3 and anti-CD28 antibodies induce transient expression of CD5L on B lymphocytes that lasts for approximately 72 h. Binding of CD5Rg to activated splenocytes is trypsin resistant and independent of divalent cations. However, it is pronase sensitive and dependent on N-linked glycosylation of CD5, since treatment of CD5Rg with PNGaseF on N-glycanase completely abrogates its ability to bind activated splenocytes. It addition to splenocytes, CD5L is expressed on activated murine T cell clones. Immunoprecipitation, antibody, and recombinant protein blocking studies indicate that CD5L is distinct from CD72, which has been proposed to be a CD5 ligand. To determine whether CD5-CD5L interaction might play a role in vivo, we tested the effect of CD5Rg in a murine model of antibody-mediated membranous glomerulonephritis. Injection of CD5Rg was found to abrogate development of the disease. Taken together, our results help identify a novel ligand of CD5 and propose a role for CD5 in the regulation of immune responses.
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1 September 1996
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September 01 1996
Identification of a novel inducible cell-surface ligand of CD5 on activated lymphocytes.
L Biancone,
L Biancone
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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M A Bowen,
M A Bowen
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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A Lim,
A Lim
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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A Aruffo,
A Aruffo
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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G Andres,
G Andres
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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I Stamenkovic
I Stamenkovic
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
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L Biancone
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
M A Bowen
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
A Lim
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
A Aruffo
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
G Andres
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
I Stamenkovic
Department of Pathology Harvard Medical School and Pathology Research, Massachusetts General Hospital, Boston 02129, USA.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1996) 184 (3): 811–819.
Citation
L Biancone, M A Bowen, A Lim, A Aruffo, G Andres, I Stamenkovic; Identification of a novel inducible cell-surface ligand of CD5 on activated lymphocytes.. J Exp Med 1 September 1996; 184 (3): 811–819. doi: https://doi.org/10.1084/jem.184.3.811
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