Your search keyword '"Cohen, Sonia"' showing total 2 results

1. MeCP2 Phosphorylation Limits Psychostimulant-Induced Behavioral and Neuronal Plasticity.

Author

Deng, Jie V., Yehong Wan, Xiaoting Wang, Cohen, Sonia, Wetsel, William C., Greenberg, Michael E., Kenny, Paul J., Calakos, Nicole, and West, Anne E.

Subjects

NUCLEUS accumbens, NEUROPLASTICITY, PHOSPHORYLATION, DNA-binding proteins, AMPHETAMINES, POST-translational modification

Abstract

he methyl-DNA binding protein MeCP2 is emerging as an important regulator of drug reinforcement processes. Psychostimulants induce phosphorylation of MeCP2 at Ser421; however, the functional significance of this posttranslational modification for addictive-like behaviors was unknown. Here we show that MeCP2 Ser421Ala knock-in mice display both a reduced threshold for the induction of locomotor sensitization by investigator-administered amphetamine and enhanced behavioral sensitivity to the reinforcing properties of self-administered cocaine. These behavioral differences were accompanied in the knock-in mice by changes in medium spiny neuron intrinsic excitability and nucleus accumbens gene expression typically observed in association with repeated exposure to these drugs. These data show that phosphorylation of MeCP2 at Ser421 functions to limit the circuit plasticities in the nucleus accumbens that underlie addictive-like behaviors. [ABSTRACT FROM AUTHOR]

Published

2014

2. Phosphorylation of MeCP2 at Ser421 Contributes to Chronic Antidepressant Action.

Author

Hutchinson, Ashley N., Deng, Jay V., Cohen, Sonia, and West, Anne E.

Subjects

THERAPEUTICS, MENTAL depression, PHOSPHORYLATION, ANTIDEPRESSANTS, TRANSCRIPTION factors, SYMPTOMS, NEURAL transmission, PROTEIN binding

Abstract

Although tricyclic antidepressants rapidly activate monoaminergic neurotransmission, these drugs must be administered chronically to alleviate symptoms of depression. This observation suggests that molecular mechanisms downstream ofmonoaminereceptor activation, which include the induction of gene transcription, underlie chronic antidepressant-induced changes in behavior. Here we show that methyl-CpG-binding protein 2 (MeCP2) regulates behavioral responses to chronic antidepressant treatment. Imipramine administration induces phosphorylation of MeCP2 at Ser421 (pMeCP2) selectively in the nucleus accumbens and the lateral habenula, two brain regions important for depressive-like behaviors. To test the role of pMeCP2 in depressive-like behaviors, we used male mice that bear a germ-line mutation knocked into the X-linked Mecp2 locus that changes Ser421 to a nonphosphorylatable Ala residue (S421A). MeCP2 S421A knock-in (KI) mice showed increased immobility in forced-swim and tail-suspension tests compared with their wild-type (WT) littermates. However, immobility of both MeCP2 WT and KI mice in forced swim was reduced by acute administration of imipramine, demonstrating that loss of pMeCP2 does not impair acute pharmacological sensitivity to this drug. After chronic social defeat stress, chronic administration of imipramine significantly improved social interaction in the MeCP2 WT mice. In contrast, the MeCP2 KI mice did not respond to chronic imipramine administration. These data suggest novel roles for pMeCP2 in the sensitivity to stressful stimuli and demonstrate that pMeCP2 is required for the effects of chronic imipramine on depressive-like behaviors induced by chronic social defeat stress. [ABSTRACT FROM AUTHOR]

Published

2012