Cell Reports (Mar 2013)

Ubiquitin C-Terminal Hydrolase-L1 Potentiates Cancer Chemosensitivity by Stabilizing NOXA

  • Kerstin Brinkmann,
  • Paola Zigrino,
  • Axel Witt,
  • Michael Schell,
  • Leena Ackermann,
  • Pia Broxtermann,
  • Stephan Schüll,
  • Maria Andree,
  • Oliver Coutelle,
  • Benjamin Yazdanpanah,
  • Jens Michael Seeger,
  • Daniela Klubertz,
  • Uta Drebber,
  • Ulrich T. Hacker,
  • Martin Krönke,
  • Cornelia Mauch,
  • Thorsten Hoppe,
  • Hamid Kashkar

DOI
https://doi.org/10.1016/j.celrep.2013.02.014
Journal volume & issue
Vol. 3, no. 3
pp. 881 – 891

Abstract

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The BH3-only protein NOXA represents one of the critical mediators of DNA-damage-induced cell death. In particular, its involvement in cellular responses to cancer chemotherapy is increasingly evident. Here, we identify a strategy of cancer cells to escape genotoxic chemotherapy by increasing proteasomal degradation of NOXA. We show that the deubiquitylating enzyme UCH-L1 is a key regulator of NOXA turnover, which protects NOXA from proteasomal degradation by removing Lys48-linked polyubiquitin chains. In the majority of tumors from patients with melanoma or colorectal cancer suffering from high rates of chemoresistance, NOXA fails to accumulate because UCH-L1 expression is epigenetically silenced. Whereas UCH-L1/NOXA-positive tumor samples exhibit increased sensitivity to genotoxic chemotherapy, downregulation of UCH-L1 or inhibition of its deubiquitylase activity resulted in reduced NOXA stability and resistance to genotoxic chemotherapy in both human and C. elegans cells. Our data identify the UCH-L1/NOXA interaction as a therapeutic target for overcoming cancer chemoresistance.