Fission yeast 26S proteasome mutants are multi-drug resistant due to stabilization of the pap1 transcription factor

A Varshavsky; C Gordon; Caroline R. Wilkinson; Christopher J. McInerny; Colin Gordon; CR Wilkinson; Deanna M. Koepp; E Strickland; H Seino; IS Nielsen; Itaru Samejima; K Nagao; M Arioka; M Penney; M Shimanuki; Mairi Wallace; Mary Penney; MH Glickman; R Booher; Rasmus Hartmann-Petersen; RJ Dohmen; S Moreno; Søs G. Mathiassen; T Toda; T Toda; Takashi Toda; TG Turi; V Bailly; WM Toone

research

Fission yeast 26S proteasome mutants are multi-drug resistant due to stabilization of the pap1 transcription factor

Authors: A Varshavsky
C Gordon
Caroline R. Wilkinson
Christopher J. McInerny
Colin Gordon
CR Wilkinson
Deanna M. Koepp
E Strickland
H Seino
IS Nielsen
Itaru Samejima
K Nagao
M Arioka
M Penney
M Shimanuki
Mairi Wallace
Mary Penney
MH Glickman
R Booher
Rasmus Hartmann-Petersen
RJ Dohmen
S Moreno
Søs G. Mathiassen
T Toda
T Toda
Takashi Toda
TG Turi
V Bailly
WM Toone
Publication date: 1 January 2012
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Here we report the result of a genetic screen for mutants resistant to the microtubule poison methyl benzimidazol-2-yl carbamate (MBC) that were also temperature sensitive for growth. In total the isolated mutants were distributed in ten complementation groups. Cloning experiments revealed that most of the mutants were in essential genes encoding various 26S proteasome subunits. We found that the proteasome mutants are multi-drug resistant due to stabilization of the stress-activated transcription factor Pap1. We show that the ubiquitylation and ultimately the degradation of Pap1 depend on the Rhp6/Ubc2 E2 ubiquitin conjugating enzyme and the Ubr1 E3 ubiquitin-protein ligase. Accordingly, mutants lacking Rhp6 or Ubr1 display drug-resistant phenotypes