Downregulation of Major Histocompatibility Complex Class I Molecules by Kaposi's Sarcoma-Associated Herpesvirus K3 and K5 Proteins

Ishido, Satoshi; Wang, Chunyang; Lee, Bok-Soo; Cohen, George B.; Jung, Jae U.

doi:10.1128/jvi.74.11.5300-5309.2000

Cited by 405 publications

(335 citation statements)

References 40 publications

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“…98 In addition, the KSHVencoded K3 and K5 proteins also differentially affect MHC class I antigen expression: the K3 protein significantly downregulates HLA-A, -B, -C and -E antigens, whereas the K5 protein selectively suppresses the expression of HLA-A and -B, but not that of HLA-E antigens. 99 This difference is attributable to altered amino acid sequences in the transmembrane region of the respective HLA class I antigens. 71 Recently, it has been shown that the HPV E5 protein specifically downregulates HLA-A and -B gene transcription.…”

Section: Hla Class I Antigen Downregulationmentioning

confidence: 99%

Molecular mechanisms of HLA class I antigen abnormalities following viral infection and transformation

Seliger

Ritz

Ferrone

2005

Intl Journal of Cancer

112

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In humans as in other animal species, CD81 cytotoxic T lymphocytes (CTLs) play an important if not the major role in controlling virus-infected and malignant cell growth. The interactions between CD81 T cells and target cells are mediated by human leukocyte antigen (HLA) class I antigens loaded with viral and tumor antigen-derived peptides along with costimulatory receptor/ligand stimuli. Thus, to escape from CD8 1 T-cell recognition and destruction, viruses and tumor cells have developed strategies to inhibit the expression and/or function of HLA class I antigens. In contrast, cells with downregulated MHC class I surface expression can be recognized by NK cells, although NK cell-mediated lysis could be abrogated by the expression of inhibiting NK cell receptors. This review discusses the molecular mechanisms utilized by viruses to inhibit the formation, transport and/or expression of HLA class I antigen/peptide complexes on the cell surface. The knowledge about viral interference with MHC class I antigen presentation is not only crucial to understand the pathogenesis of viral diseases, but contributes also to the design of novel strategies to counteract the escape mechanisms utilized by viruses. These investigations may eventually lead to the development of effective immunotherapies to control viral infections and virus-associated malignant diseases. ' 2005 Wiley-Liss, Inc.

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Section: Hla Class I Antigen Downregulationmentioning

confidence: 99%

Molecular mechanisms of HLA class I antigen abnormalities following viral infection and transformation

Seliger

Ritz

Ferrone

2005

Intl Journal of Cancer

112

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“…MIR family proteins bind to the membrane through their hydrophobic domains located at the center and possess two intracellular regions. The initially discovered MIR family proteins are viral E3s: MIR1 and MIR2 of Kaposi's sarcoma-associated herpesvirus (KSHV), mK3 of murine ␥-herpesvirus 68, and m153R of myxomavirus (3,(5)(6)(7)(8)(9). Each molecule targets a different set of Ag presentation-related molecules: CD1d and MHC class I (MHC I) for MIR1; B7-2, ICAM-1, CD1d, and MHC I for MIR2; MHC I for mK3; MHC I, CD4, and Fas for m153R (3, 5, 9 -12).…”

Section: Inhibition Of Mhc Class II Expression and Immune Responses Bmentioning

confidence: 99%

Inhibition of MHC Class II Expression and Immune Responses by c-MIR

Ohmura‐Hoshino

Matsuki

Aoki

et al. 2006

The Journal of Immunology

Self Cite

124

118

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We previously reported a novel E3 ubiquitin ligase (E3), designated as c-MIR, which targets B7-2 to lysosomal degradation and down-regulates the B7-2 surface expression through ubiquitination of its cytoplasmic tail. B7-2 is well known as a costimulatory molecule for Ag presentation, suggesting that the manipulation of c-MIR expression modulates immune responses in vivo. To examine this hypothesis, we generated genetically modified mice in which c-MIR was expressed under an invariant chain (Ii) promoter. Dendritic cells derived from genetically engineered mice showed low ability to present Ags. In addition, these mice showed resistance to the onset of experimental autoimmune encephalomyelitis and an impaired development of CD4 T cells in the thymus and the periphery. These findings led us to conclude that MHC class II (MHC II) is an additional target for c-MIR. Indeed, forced expression of c-MIR in several B cell lines down-regulated the surface expression of MHC II, and down-regulation was found to depend on the presence of a single lysine residue in the cytoplasmic tail of the I-A β-chain. In a reconstitution system using 293T cells, we found that the lysine residue at position 225 in the I-A β-chain was ubiquitinated by c-MIR. To our knowledge, c-MIR is the first example of an E3 that is capable of inhibiting MHC II expression. Our findings suggest that c-MIR might potently regulate immune responses in vivo.

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“…They function as membrane-bound ubiquitin ligases, leading to ubiquitination of their target proteins on lysine residues in their cytosolic tails (32). The result of this ubiquitination is the enhancement of the endocytosis of the target chain and its delivery (via the multivesicular body) to the lysosome, where it is proteolytically destroyed (28,30). Both MIR1 and MIR2 reduce the cell surface levels of MHC class I; MIR2 also selectively targets the costimulatory molecules B7.2 and ICAM-1, both of which are involved in the enhancement of helper T cell signaling (33,34).…”

Section: Introductionmentioning

confidence: 99%

“…[25][26][27]. Like other herpesvirus family members, it encodes proteins that block MHC class I expression on the cell surface (28)(29)(30)(31). These are known as modulator of immune recognition (MIR) proteins; MIR1 and MIR2 are expressed during lytic replication and are encoded by the open reading frames K3 and K5, respectively.…”

Section: Introductionmentioning

confidence: 99%