OncoImmunology (Jan 2018)

Deubiquitinases A20 and CYLD modulate costimulatory signaling via CD137 (4–1BB)

  • Arantza Azpilikueta,
  • Elixabet Bolaños,
  • Valerie Lang,
  • Sara Labiano,
  • Maria A. Aznar,
  • Iñaki Etxeberria,
  • Alvaro Teijeira,
  • Maria E. Rodriguez-Ruiz,
  • Jose L. Perez-Gracia,
  • Maria Jure-Kunkel,
  • Juan M. Zapata,
  • Manuel S. Rodriguez,
  • Ignacio Melero

DOI
https://doi.org/10.1080/2162402X.2017.1368605
Journal volume & issue
Vol. 7, no. 1

Abstract

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TRAF2 dependent K63-polyubiquitinations have been recently shown to connect CD137 (4–1BB) stimulation to NF-κB activation. In a search of deubiquitinase enzymes (DUBs) that could regulate such a signaling route, A20 and CYLD were found to coimmunoprecipitate with CD137 and TRAF2 complexes. Indeed, overexpression of A20 or CYLD downregulated CD137-elicited ubiquitination of TRAF2 and TAK1 upon stimulation with agonist monoclonal antibodies. Moreover, overexpression of A20 or CYLD downregulated CD137-induced NF-κB activation in cultured cells and in gene-transferred hepatocytes in vivo, while silencing these deubiquitinases enhanced CD137 costimulation of primary human CD8 T cells. Therefore A20 and CYLD directly downregulate the signaling from a T and NK-cell costimulatory receptor under exploitation for cancer immunotherapy in clinical trials.

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