eLife (Aug 2016)

Impairment of cocaine-mediated behaviours in mice by clinically relevant Ras-ERK inhibitors

  • Alessandro Papale,
  • Ilaria Maria Morella,
  • Marzia Tina Indrigo,
  • Rick Eugene Bernardi,
  • Livia Marrone,
  • Francesca Marchisella,
  • Andrea Brancale,
  • Rainer Spanagel,
  • Riccardo Brambilla,
  • Stefania Fasano

DOI
https://doi.org/10.7554/eLife.17111
Journal volume & issue
Vol. 5

Abstract

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Ras-ERK signalling in the brain plays a central role in drug addiction. However, to date, no clinically relevant inhibitor of this cascade has been tested in experimental models of addiction, a necessary step toward clinical trials. We designed two new cell-penetrating peptides - RB1 and RB3 - that penetrate the brain and, in the micromolar range, inhibit phosphorylation of ERK, histone H3 and S6 ribosomal protein in striatal slices. Furthermore, a screening of small therapeutics currently in clinical trials for cancer therapy revealed PD325901 as a brain-penetrating drug that blocks ERK signalling in the nanomolar range. All three compounds have an inhibitory effect on cocaine-induced ERK activation and reward in mice. In particular, PD325901 persistently blocks cocaine-induced place preference and accelerates extinction following cocaine self-administration. Thus, clinically relevant, systemically administered drugs that attenuate Ras-ERK signalling in the brain may be valuable tools for the treatment of cocaine addiction.

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