LMP1 Transmembrane Domain 1 and 2 (TM1-2) FWLY Mediates Intermolecular Interactions with TM3-6 To Activate NF-κB

Author:

Soni Vishal1,Yasui Teruhito1,Cahir-McFarland Ellen1,Kieff Elliott1

Affiliation:

1. Channing Laboratory and Infectious Disease Division, Department of Medicine, Brigham and Women's Hospital, and Department of Microbiology and Molecular Genetics, Harvard Medical School and Harvard University, 181 Longwood Avenue, Boston, Massachusetts 02115

Abstract

ABSTRACT The Epstein-Barr virus oncoprotein LMP1 has six transmembrane domains (TMs) that enable intermolecular aggregation and constitutive signaling through two C-terminal cytosolic domains. Expression of both TMs 1 and 2 without the C terminus (TM1-2ΔC) and TMs 3 to 6 fused to the C terminus (TM3-6) results in partial association, which is substantially decreased by TM1 F 38 WLY 41 mutation to A 38 ALA 41 . We now investigate whether TM1-2ΔC can functionally interact with TM3-6. TM1-2ΔC induced TM3-6 to mediate NF-κB activation at 59% of LMP1 levels, and the effect was dependent on TM1-2 F 38 WLY 41 . TM1-2ΔC even induced TM3-4 C terminus-mediated NF-κB activation to 44% of LMP1 levels. Surprisingly, this effect was TM1 F 38 WLY 41 independent, indicative of a role for TMs 5 and 6 in TM1 F 38 WLY 41 effects. TM3 W 98 was also important for TM1-2ΔC induction of TM3-6-mediated NF-κB activation, for association, and for TM1 F 38 WLY 41 dependence on C-terminal NF-κB activation. These data support models in which the TM1 F 38 WLY 41 effects are at least partially dependent on TM3 W 98 and a residue(s) in TMs 5 and 6.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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