Model for the Interaction of Gammaherpesvirus 68 RING-CH Finger Protein mK3 with Major Histocompatibility Complex Class I and the Peptide-Loading Complex

doi:10.1128/JVI.78.16.8673-8686.2004

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Journal of Virology, August 2004, p. 8673-8686, Vol. 78, No. 16
0022-538X/04/$08.00+0 DOI: 10.1128/JVI.78.16.8673-8686.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

Model for the Interaction of Gammaherpesvirus 68 RING-CH Finger Protein mK3 with Major Histocompatibility Complex Class I and the Peptide-Loading Complex

Xiaoli Wang,¹ Lonnie Lybarger,¹^, Rose Connors,¹ Michael R. Harris,² and Ted H. Hansen¹^*

Department of Pathology and Immunology,¹ Department of Pediatrics, Washington University School of Medicine, St. Louis, Missouri 63110²

Received 17 February 2004/ Accepted 12 May 2004

The mK3 protein of gammaherpesvirus 68 and the kK5 protein ofKaposi's sarcoma-associated herpesvirus are members of a familyof structurally related viral immune evasion molecules thatall possess a RING-CH domain with ubiquitin ligase activity.These proteins modulate the expression of major histocompatibilitycomplex class I molecules (mK3 and kK5) as well as other moleculeslike ICAM-1 and B7.2 (kK5). Previously, mK3 was shown to ubiquitinatenascent class I molecules, resulting in their rapid degradation,and this process was found to be dependent on TAP and tapasin,endoplasmic reticulum molecules involved in class I assembly.Here, we demonstrate that in murine cells, kK5 does not affectclass I expression but does downregulate human B7.2 moleculesin a TAP/tapasin-independent manner. These differences in substratespecificity and TAP/tapasin dependence between mK3 and kK5 permittedus, using chimeric molecules, to map the sites of mK3 interactionwith TAP/tapasin and to determine the requirements for substraterecognition by mK3. Our findings indicate that mK3 interactswith TAP1 and -2 via their C-terminal domains and with classI molecules via their N-terminal domains. Furthermore, by orientingthe RING-CH domain of mK3 appropriately with respect to classI, mK3 binding to TAP/tapasin, rather than the presence of uniquesequences in class I, appears to be the primary determinantof substrate specificity.

* Corresponding author. Mailing address: Department of Pathology and Immunology, Box 8118, Washington University School of Medicine, 4566 Scott Ave., St. Louis, MO 63110. Phone: (314) 362-2716. Fax: (314) 362-4137. E-mail: hansen{at}genetics.wustl.edu.

Present address: Department of Cell Biology and Anatomy, ArizonaHealth Sciences Center, Tucson, AZ 85724.

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