Five CD1 molecules are expressed in humans and it is unclear whether they have specialized or redundant functions. We found that sulfatide is a promiscuous CD1-binding ligand and have isolated T cell clones that are specific for sulfatide and restricted by distinct CD1 molecules. These clones have been used to compare the capacity of different CD1 to present the same glycolipid, to induce effector functions, and to form persistent immunogenic complexes. CD1a, CD1b, and CD1c molecules similarly load sulfatide on the cell surface without processing, and prime Th1 and Th2 responses. Stimulation by sulfatide-loaded CD1a persists much longer than that by CD1b and CD1c in living cells. Use of recombinant soluble CD1a confirmed the prolonged capacity to stimulate T cells. Moreover, other glycosphingolipids bind to all CD1, which suggests the presence of additional promiscuous ligands. Thus, group I CD1 molecules present an overlapping set of self-glycolipids, even though they are quite divergent from an evolutionary point of view.
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15 April 2002
Article|
April 08 2002
Presentation of the Same Glycolipid by Different CD1 Molecules
A. Shamshiev,
A. Shamshiev
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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H.-J. Gober,
H.-J. Gober
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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A. Donda,
A. Donda
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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Z. Mazorra,
Z. Mazorra
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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L. Mori,
L. Mori
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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G. De Libero
G. De Libero
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
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A. Shamshiev
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
H.-J. Gober
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
A. Donda
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
Z. Mazorra
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
L. Mori
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
G. De Libero
Experimental Immunology, Department of Research, University Hospital, 4031 Basel, Switzerland
Address correspondence to Gennaro De Libero, Experimental Immunology, Department of Research, University Hospital, Hebelstrasse 20, 4031 Basel, Switzerland. Phone: 41-61-265-23-27; Fax: 41-61-265-23-50; E-mail: [email protected]
A. Shamshiev and H.-J. Gober contributed equally to this work.
*
Abbreviations used in this paper: β2m, β2 microglobulin; DC, dendritic cells; GalCer, galactosylceramide; GlcCer, glucosylceramide; LacCer, lactosylceramide; PPD, purified protein derivative; sCD1a, soluble CD1a.
Received:
November 25 2001
Revision Received:
February 13 2002
Accepted:
February 28 2002
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2002
J Exp Med (2002) 195 (8): 1013–1021.
Article history
Received:
November 25 2001
Revision Received:
February 13 2002
Accepted:
February 28 2002
Citation
A. Shamshiev, H.-J. Gober, A. Donda, Z. Mazorra, L. Mori, G. De Libero; Presentation of the Same Glycolipid by Different CD1 Molecules . J Exp Med 15 April 2002; 195 (8): 1013–1021. doi: https://doi.org/10.1084/jem.20011963
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