Viral Degradation of the MHC Class I Peptide Loading Complex

Viral Degradation of the MHC Class I Peptide Loading Complex

The murine γ-herpesvirus-68 MK3 protein inhibits CD8 + T cell recognition by ubiquitinating the cytoplasmic tails of classical MHC class I heavy chains. Here we show that MK3 also provides the first example of a protein that degrades tapasin and TAP. The degradation was MK3 RING finger dependent and...

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Veröffentlicht in:Immunity (Cambridge, Mass.) Mass.), 2004-03, Vol.20 (3), p.305-317
Hauptverfasser: Boname, Jessica M., de Lima, Brigitte D., Lehner, Paul J., Stevenson, Philip G.
Format: Artikel
Sprache:eng
Schlagworte:
Animals
ATP Binding Cassette Transporter, Subfamily B, Member 3
ATP-Binding Cassette Transporters - physiology
Biological Transport
CD8-Positive T-Lymphocytes - immunology
CD8-Positive T-Lymphocytes - virology
Cell Line
Colleges & universities
Down-Regulation
Herpesvirus
Histocompatibility Antigens Class I - metabolism
Immune system
Interferon-gamma - pharmacology
Lymphocytes
Macromolecular Substances
Mice
MK3 protein
Peptides
Peptides - metabolism
Proteins
Rhadinovirus - pathogenicity
Ubiquitins - metabolism
Viral Proteins - metabolism
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Zusammenfassung:The murine γ-herpesvirus-68 MK3 protein inhibits CD8 + T cell recognition by ubiquitinating the cytoplasmic tails of classical MHC class I heavy chains. Here we show that MK3 also provides the first example of a protein that degrades tapasin and TAP. The degradation was MK3 RING finger dependent and primarily affected TAP. MK3 associated with TAP1 in the absence of tapasin or TAP2, suggesting that TAP1 was a primary binding partner in the peptide loading complex. TAP2 also played a major role in MK3 stability and function. By degrading TAP, therefore, MK3 limited its own expression. However, TAP degradation also broadened the MK3 inhibitory repertoire and achieved a remarkable resistance to MHC class I upregulation by interferon-γ, suggesting that it represents a specific adaptation to immune evasion in lymphoid tissue.
ISSN:1074-7613
1097-4180
DOI:10.1016/S1074-7613(04)00047-0