PLoS ONE (Jan 2015)

PSMC5, a 19S Proteasomal ATPase, Regulates Cocaine Action in the Nucleus Accumbens.

  • Yoko H Ohnishi,
  • Yoshinori N Ohnishi,
  • Takanori Nakamura,
  • Mizuki Ohno,
  • Pamela J Kennedy,
  • Yasuyuki Ohkawa,
  • Akinori Nishi,
  • Rachael Neve,
  • Teruhisa Tsuzuki,
  • Eric J Nestler

DOI
https://doi.org/10.1371/journal.pone.0126710
Journal volume & issue
Vol. 10, no. 5
p. e0126710

Abstract

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ΔFosB is a stable transcription factor which accumulates in the nucleus accumbens (NAc), a key part of the brain's reward circuitry, in response to chronic exposure to cocaine or other drugs of abuse. While ΔFosB is known to heterodimerize with a Jun family member to form an active transcription factor complex, there has not to date been an open-ended exploration of other possible binding partners for ΔFosB in the brain. Here, by use of yeast two-hybrid assays, we identify PSMC5-also known as SUG1, an ATPase-containing subunit of the 19S proteasomal complex-as a novel interacting protein with ΔFosB. We verify such interactions between endogenous ΔFosB and PSMC5 in the NAc and demonstrate that both proteins also form complexes with other chromatin regulatory proteins associated with gene activation. We go on to show that chronic cocaine increases nuclear, but not cytoplasmic, levels of PSMC5 in the NAc and that overexpression of PSMC5 in this brain region promotes the locomotor responses to cocaine. Together, these findings describe a novel mechanism that contributes to the actions of ΔFosB and, for the first time, implicates PSMC5 in cocaine-induced molecular and behavioral plasticity.