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Promiscuity of MCMV immunoevasin of NKG2D: m138/fcr-1 down-modulates RAE-1epsilon in addition to MULT-1 and H60 (CROSBI ID 158493)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Arapović, Jurica ; Lenac Roviš, Tihana ; Reddy, A.B. ; Krmpotić, Astrid ; Jonjić, Stipan Promiscuity of MCMV immunoevasin of NKG2D: m138/fcr-1 down-modulates RAE-1epsilon in addition to MULT-1 and H60 // Molecular immunology, 47 (2009), 1; 114-122. doi: 10.1016/j.molimm.2009.02.010

Podaci o odgovornosti

Arapović, Jurica ; Lenac Roviš, Tihana ; Reddy, A.B. ; Krmpotić, Astrid ; Jonjić, Stipan

engleski

Promiscuity of MCMV immunoevasin of NKG2D: m138/fcr-1 down-modulates RAE-1epsilon in addition to MULT-1 and H60

Both human and mouse cytomegalovirus (CMV) encode proteins that inhibit the activation of NK cells by down-regulating the cellular ligands for activating NK cell receptor, NKG2D. MCMV proteins m145, m152 and m155 interfere with the expression of all known NKG2D ligands, MULT-1, RAE-1 family members and H60, respectively, whereas m138 affects the expression of MULT-1 and H60. Here we show that m152 affects the maturation of newly synthesized RAE-1 molecules, but is not sufficient to prevent surface expression of RAE-1varepsilon. We have identified m138 as a main inhibitor of the surface expression of RAE-1varepsilon. In contrast to m152, m138 affects the surface-resident protein leading to its endocytosis, which can be prevented by a dynamin inhibitor. Moreover, we demonstrated that m138 does not need other viral proteins to down-modulate the expression of RAE-1varepsilon.

mouse cytomegalovirus; NK cells; Immunoevasion; NKG2D; RAE-1

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Podaci o izdanju

47 (1)

2009.

114-122

objavljeno

0161-5890

10.1016/j.molimm.2009.02.010

Povezanost rada

Temeljne medicinske znanosti

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