Differential Susceptibility of RAE-1 Isoforms to Mouse Cytomegalovirus

Author:

Arapović Jurica1,Lenac Tihana1,Antulov Ronald1,Polić Bojan1,Ruzsics Zsolt2,Carayannopoulos Leonidas N.3,Koszinowski Ulrich H.2,Krmpotić Astrid1,Jonjić Stipan1

Affiliation:

1. Department of Histology and Embryology, Medical Faculty University of Rijeka, 51000 Rijeka, Croatia

2. Max von Pettenkofer Institute, LMU, 80336 Munich, Germany

3. Division of Pulmonary and Critical Care Medicine, Washington University School of Medicine, St. Louis, Missouri 63110

Abstract

ABSTRACT The NKG2D receptor is one of the most potent activating natural killer cell receptors involved in antiviral responses. The mouse NKG2D ligands MULT-1, RAE-1, and H60 are regulated by murine cytomegalovirus (MCMV) proteins m145, m152, and m155, respectively. In addition, the m138 protein interferes with the expression of both MULT-1 and H60. We show here that one of five RAE-1 isoforms, RAE-1δ, is resistant to downregulation by MCMV and that this escape has functional importance in vivo. Although m152 retained newly synthesized RAE-1δ and RAE-1γ in the endoplasmic reticulum, no viral regulator was able to affect the mature RAE-1δ form which remains expressed on the surfaces of infected cells. This differential susceptibility to downregulation by MCMV is not a consequence of faster maturation of RAE-1δ compared to RAE-1γ but rather an intrinsic property of the mature surface-resident protein. This difference can be attributed to the absence of a PLWY motif from RAE-1δ. Altogether, these findings provide evidence for a novel mechanism of host escape from viral immunoevasion of NKG2D-dependent control.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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