Therefore, HDAC inhibitors might reactivate the expression of plasticity-related genes in the adult cortex by enhancing CREB-mediated gene transcription. This possibility is also supported by the observation that MD in adult mice triggers selleck screening library a labile form of plasticity that can be rendered persistent by the expression of a constitutively active CREB mutant (Pham et al., 2004). Which genes are crucially involved in mediating the action of HDAC inhibitors on visual cortical plasticity, or in other models of brain plasticity, is still poorly known. Further analyses are required to unravel the final effectors of the epigenetic treatment on visual
cortical plasticity (Borrelli et al., 2008; Fagiolini et al., 2009). In addition learn more to the manipulation of epigenetic mechanisms, other factors are able to promote a recovery from amblyopia in adult rodents. Environmental enrichment (Sale et al., 2007) and dark rearing (He et al., 2007), coupled with RS or binocular vision, allow the recovery of a long-term deprived eye to normal levels of acuity and ocular dominance. Both protocols lead to a reduction in GABAergic inhibition and
probably result in a return to an SP-like balance between excitation and inhibition (Spolidoro et al., 2009). Influencing specific molecular and cellular components was also found to promote recovery from amblyopia in adulthood. Visual cortical plasticity is inhibited by the aggregation of extracellular matrix molecules such as chondroitin sulphate proteoglycans (CSPGs). Enzymatic digestion of CSPGs in combination with RS has been shown to restore visual cortical plasticity in adult rats (Pizzorusso et al., 2002) and to reverse the effects of long-term MD on visual acuity and ocular dominance (Pizzorusso et al., 2006). Also, chronic administration of fluoxetine (which increases extracellular serotonin levels), coupled with RS, allows visual acuity and ocular dominance
recovery from long-term MD (Maya Vetencourt Sorafenib et al., 2008); again, a possible mediator of the effect is the lowering of the inhibitory tone (Spolidoro et al., 2009). Intriguingly, environmental enrichment induces histone acetylation, and fluoxetine causes alterations in gene expression overlapping with those induced by HDAC inhibitor treatment (Fischer et al., 2007; Covington et al., 2009); it is therefore possible that epigenetic mechanisms could represent a common endpoint of other treatments enhancing plasticity in the adult visual cortex (Pizzorusso et al., 2007). In summary, our study demonstrates that targeting HDACs can be an effective pharmacological strategy to promote experience-dependent plasticity in the adult visual cortex and recovery from amblyopia.