Epstein-Barr virus-driven B cell lymphoma mediated by a direct LMP1-TRAF6 complex

Fabian Giehler; Michael S Ostertag; Thomas Sommermann; Daniel Weidl; Kai R Sterz; Helmut Kutz; Andreas Moosmann; Stephan M Feller; Arie Geerlof; Brigitte Biesinger; Grzegorz M Popowicz; Johannes Kirchmair; Arnd Kieser

doi:10.1038/s41467-023-44455-w

Epstein-Barr virus-driven B cell lymphoma mediated by a direct LMP1-TRAF6 complex

Fabian Giehler
, Michael S Ostertag
, Thomas Sommermann
, Daniel Weidl
, Kai R Sterz
, Helmut Kutz
, Andreas Moosmann
, Stephan M Feller
, Arie Geerlof
, Brigitte Biesinger
, Grzegorz M Popowicz
, Johannes Kirchmair
, Arnd Kieser

Department of Pharmaceutical Sciences

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

Epstein-Barr virus (EBV) latent membrane protein 1 (LMP1) drives viral B cell transformation and oncogenesis. LMP1's transforming activity depends on its C-terminal activation region 2 (CTAR2), which induces NF-κB and JNK by engaging TNF receptor-associated factor 6 (TRAF6). The mechanism of TRAF6 recruitment to LMP1 and its role in LMP1 signalling remains elusive. Here we demonstrate that TRAF6 interacts directly with a viral TRAF6 binding motif within CTAR2. Functional and NMR studies supported by molecular modeling provide insight into the architecture of the LMP1-TRAF6 complex, which differs from that of CD40-TRAF6. The direct recruitment of TRAF6 to LMP1 is essential for NF-κB activation by CTAR2 and the survival of LMP1-driven lymphoma. Disruption of the LMP1-TRAF6 complex by inhibitory peptides interferes with the survival of EBV-transformed B cells. In this work, we identify LMP1-TRAF6 as a critical virus-host interface and validate this interaction as a potential therapeutic target in EBV-associated cancer.

Original language	English
Article number	414
Journal	Nature Communications
Volume	15
Issue number	1
DOIs	https://doi.org/10.1038/s41467-023-44455-w
Publication status	Published - 10 Jan 2024

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Austrian Fields of Science 2012

106005 Bioinformatics
301207 Pharmaceutical chemistry

Keywords

Humans
Herpesvirus 4, Human
TNF Receptor-Associated Factor 6
Epstein-Barr Virus Infections/complications
NF-kappa B
Cell Transformation, Neoplastic
Cell Transformation, Viral
Lymphoma, B-Cell

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title = "Epstein-Barr virus-driven B cell lymphoma mediated by a direct LMP1-TRAF6 complex",

abstract = "Epstein-Barr virus (EBV) latent membrane protein 1 (LMP1) drives viral B cell transformation and oncogenesis. LMP1's transforming activity depends on its C-terminal activation region 2 (CTAR2), which induces NF-κB and JNK by engaging TNF receptor-associated factor 6 (TRAF6). The mechanism of TRAF6 recruitment to LMP1 and its role in LMP1 signalling remains elusive. Here we demonstrate that TRAF6 interacts directly with a viral TRAF6 binding motif within CTAR2. Functional and NMR studies supported by molecular modeling provide insight into the architecture of the LMP1-TRAF6 complex, which differs from that of CD40-TRAF6. The direct recruitment of TRAF6 to LMP1 is essential for NF-κB activation by CTAR2 and the survival of LMP1-driven lymphoma. Disruption of the LMP1-TRAF6 complex by inhibitory peptides interferes with the survival of EBV-transformed B cells. In this work, we identify LMP1-TRAF6 as a critical virus-host interface and validate this interaction as a potential therapeutic target in EBV-associated cancer.",

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AU - Giehler, Fabian

AU - Ostertag, Michael S

AU - Sommermann, Thomas

AU - Weidl, Daniel

AU - Sterz, Kai R

AU - Kutz, Helmut

AU - Moosmann, Andreas

AU - Feller, Stephan M

AU - Geerlof, Arie

AU - Biesinger, Brigitte

AU - Popowicz, Grzegorz M

AU - Kirchmair, Johannes

AU - Kieser, Arnd

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AB - Epstein-Barr virus (EBV) latent membrane protein 1 (LMP1) drives viral B cell transformation and oncogenesis. LMP1's transforming activity depends on its C-terminal activation region 2 (CTAR2), which induces NF-κB and JNK by engaging TNF receptor-associated factor 6 (TRAF6). The mechanism of TRAF6 recruitment to LMP1 and its role in LMP1 signalling remains elusive. Here we demonstrate that TRAF6 interacts directly with a viral TRAF6 binding motif within CTAR2. Functional and NMR studies supported by molecular modeling provide insight into the architecture of the LMP1-TRAF6 complex, which differs from that of CD40-TRAF6. The direct recruitment of TRAF6 to LMP1 is essential for NF-κB activation by CTAR2 and the survival of LMP1-driven lymphoma. Disruption of the LMP1-TRAF6 complex by inhibitory peptides interferes with the survival of EBV-transformed B cells. In this work, we identify LMP1-TRAF6 as a critical virus-host interface and validate this interaction as a potential therapeutic target in EBV-associated cancer.

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KW - TNF Receptor-Associated Factor 6

KW - Epstein-Barr Virus Infections/complications

KW - NF-kappa B

KW - Cell Transformation, Neoplastic

KW - Cell Transformation, Viral

KW - Lymphoma, B-Cell

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Epstein-Barr virus-driven B cell lymphoma mediated by a direct LMP1-TRAF6 complex

Abstract

UN SDGs

Austrian Fields of Science 2012

Keywords

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