Cell surface proteins major histocompatibility complex (MHC) class I–related chain A (MICA) and UL16-binding proteins (ULBP) 1, 2, and 3 are up-regulated upon infection or tumor transformation and can activate human natural killer (NK) cells. Patches of cross-linked raft resident ganglioside GM1 colocalized with ULBP1, 2, 3, or MICA, but not CD45. Thus, ULBPs and MICA are expressed in lipid rafts at the cell surface. Western blotting revealed that glycosylphosphatidylinositol (GPI)-anchored ULBP3 but not transmembrane MICA, MHC class I protein, or transferrin receptor, accumulated in detergent-resistant membranes containing GM1. Thus, MICA may have a weaker association with lipid rafts than ULBP3, yet both proteins accumulate at an activating human NK cell immune synapse. Target cell lipid rafts marked by green fluorescent protein–tagged GPI also accumulate with ULBP3 at some synapses. Electron microscopy reveals constitutive clusters of ULBP at the cell surface. Regarding a specific molecular basis for the organization of these proteins, ULBP1, 2, and 3 and MICA are lipid modified. ULBP1, 2, and 3 are GPI anchored, and we demonstrate here that MICA is S-acylated. Finally, expression of a truncated form of MICA that lacks the putative site for S-acylation and the cytoplasmic tail can be expressed at the cell surface, but is unable to activate NK cells.
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5 April 2004
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March 29 2004
Cell Surface Organization of Stress-inducible Proteins ULBP and MICA That Stimulate Human NK Cells and T Cells via NKG2D
Konstantina Eleme,
Konstantina Eleme
1Department of Biological Sciences
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Sabrina B. Taner,
Sabrina B. Taner
1Department of Biological Sciences
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Björn Önfelt,
Björn Önfelt
1Department of Biological Sciences
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Lucy M. Collinson,
Lucy M. Collinson
1Department of Biological Sciences
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Fiona E. McCann,
Fiona E. McCann
1Department of Biological Sciences
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N. Jan Chalupny,
N. Jan Chalupny
3Amgen, Seattle, WA 98101
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Colin Hopkins,
Colin Hopkins
1Department of Biological Sciences
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Anthony I. Magee,
Anthony I. Magee
2Department of Biomedical Sciences, Imperial College, London SW7 2AZ, UK
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Daniel M. Davis
Daniel M. Davis
1Department of Biological Sciences
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Konstantina Eleme
1Department of Biological Sciences
Sabrina B. Taner
1Department of Biological Sciences
Björn Önfelt
1Department of Biological Sciences
Lucy M. Collinson
1Department of Biological Sciences
Fiona E. McCann
1Department of Biological Sciences
N. Jan Chalupny
3Amgen, Seattle, WA 98101
David Cosman
3Amgen, Seattle, WA 98101
Colin Hopkins
1Department of Biological Sciences
Anthony I. Magee
2Department of Biomedical Sciences, Imperial College, London SW7 2AZ, UK
Daniel M. Davis
1Department of Biological Sciences
Address correspondence to Daniel M. Davis, Dept. of Biological Sciences, Sir Alexander Fleming Building, Imperial College, London SW7 2AZ, UK. Phone: 44-207-594-5420; Fax: 44-207-594-3044; email: [email protected]
K. Eleme, S.B. Taner, and B. Önfelt contributed equally to this work.
Received:
December 18 2003
Accepted:
February 05 2004
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2004
J Exp Med (2004) 199 (7): 1005–1010.
Article history
Received:
December 18 2003
Accepted:
February 05 2004
Citation
Konstantina Eleme, Sabrina B. Taner, Björn Önfelt, Lucy M. Collinson, Fiona E. McCann, N. Jan Chalupny, David Cosman, Colin Hopkins, Anthony I. Magee, Daniel M. Davis; Cell Surface Organization of Stress-inducible Proteins ULBP and MICA That Stimulate Human NK Cells and T Cells via NKG2D . J Exp Med 5 April 2004; 199 (7): 1005–1010. doi: https://doi.org/10.1084/jem.20032194
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