Brain-Specific Phosphorylation of MeCP2 Regulates Activity-Dependent Bdnf Transcription, Dendritic Growth, and Spine Maturation

Zhou, Zhaolan; Hong, Elizabeth J.; Cohen, Sonia; Zhao, Wenqian; Ho, Hsin‐Yi Henry; Schmidt, Lauren; Chen, Wen G.; Lin, Yingxi; Savner, Erin M.; Griffith, Eric C.; Hu, Linda; Steen, Judith A.; Weitz, Charles J.; Greenberg, Michael E.

doi:10.1016/j.neuron.2006.09.037

Cited by 762 publications

(896 citation statements)

References 53 publications

(55 reference statements)

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“…44 On the other hand, BDNF promoter IV binds the transcriptional repressor, MeCP2 (a methyl-CpG-binding domain protein), in complex with the corepressor sin3a and HDACs. [45][46][47] Inhibition of HDAC by VPA or other inhibitors could cause dissociation of the repressor-corepressor complex from the promoter, resulting in transcriptional disinhibition. It is noteworthy that the antidepressant effect of imipramine is largely reversed by HDAC5 overexpression in the hippocampus of mice subjected to chronic defeat stress, which per se induces downregulation of BDNF III and IV mRNA.…”

Section: Discussionmentioning

confidence: 99%

The mood stabilizers lithium and valproate selectively activate the promoter IV of brain-derived neurotrophic factor in neurons

et al. 2007

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Brain-derived neurotrophic factor (BDNF) has been strongly implicated in the synaptic plasticity, neuronal survival and pathophysiology of depression. Lithium and valproic acid (VPA) are two primary mood-stabilizing drugs used to treat bipolar disorder. Treatment of cultured rat cortical neurons with therapeutic concentrations of LiCl or VPA selectively increased the levels of exon IV (formerly rat exon III)-containing BDNF mRNA, and the activity of BDNF promoter IV. Surprisingly, lithium-or VPA-responsive element(s) in promoter IV resides in a region upstream from the calcium-responsive elements (CaREs) responsible for depolarization-induced BDNF induction. Moreover, activation of BDNF promoter IV by lithium or VPA occurred in cortical neurons depolarized with KCl, and deletion of these three CaREs did not abolish lithium-or VPA-induced activation. Lithium and VPA are direct inhibitors of glycogen synthase kinase-3 (GSK-3) and histone deacetylase (HDAC), respectively. We showed that lithium-induced activation of promoter IV was mimicked by pharmacological inhibition of GSK-3 or short interfering RNA (siRNA)-mediated gene silencing of GSK-3a or GSK-3b isoforms. Furthermore, treatment with other HDAC inhibitors, sodium butyrate and trichostatin A, or transfection with an HDAC1-specific siRNA also activated BDNF promoter IV. Our study demonstrates for the first time that GSK-3 and HDAC are respective initial targets for lithium and VPA to activate BDNF promoter IV, and that this BDNF induction involves a novel responsive region in promoter IV of the BDNF gene. Our results have strong implications for the therapeutic actions of these two mood stabilizers.

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Section: Discussionmentioning

confidence: 99%

The mood stabilizers lithium and valproate selectively activate the promoter IV of brain-derived neurotrophic factor in neurons

et al. 2007

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“…345 There are also reports that Mecp2 plays a role in the regulation of Bdnf levels. 134,201,202 Reduction in the levels of Bdnf exacerbates the phenotype of both the Rett syndrome-model mouse 346 and the Sert deletion line. [208][209][210] In the Rett syndrome-model mouse, Bdnf overexpression with an inducible Bdnf transgene leads to partial correction of abnormalities linked to loss of Mecp2 function.…”

Section: Discussionmentioning

confidence: 99%

“…One study demonstrated that Mecp2 regulation of dendritic patterning and other components of neuronal connectivity is dependent on phosphorylation induced by neuronal activation. 134 The application of a selective CaMKII inhibitor, but not inhibitors of other kinases (CaMKK, protein kinase A, protein kinase C, mitogen-activated protein kinase, cyclin-dependent kinase 5 (CDK5), or phosphatidylinositol 3-kinase (PI3K)), blocked the stimulation-dependent phosphorylation of Mecp2, suggesting that CaMKII modulates the state of Mecp2 activation during synaptic transmission. 134 In addition to altered translation, dysregulation of CaMKII could occur through processes involved in autophosphorylation.…”

Section: Mouse Models Of Genetic Clinical Disorders With Autism Symptmentioning

confidence: 99%

“…134 The application of a selective CaMKII inhibitor, but not inhibitors of other kinases (CaMKK, protein kinase A, protein kinase C, mitogen-activated protein kinase, cyclin-dependent kinase 5 (CDK5), or phosphatidylinositol 3-kinase (PI3K)), blocked the stimulation-dependent phosphorylation of Mecp2, suggesting that CaMKII modulates the state of Mecp2 activation during synaptic transmission. 134 In addition to altered translation, dysregulation of CaMKII could occur through processes involved in autophosphorylation. Weeber et al 116 have reported that Ube3A (mÀ/p þ ) mice have higher levels of aCaMKII phosphorylation at a site inhibitory for enzymatic activity.…”

Section: Mouse Models Of Genetic Clinical Disorders With Autism Symptmentioning

confidence: 99%

“…[192][193][194] Work with mouse lines characterized by deficient Bdnf has shown that these trophic effects are important for normal serotonergic neurotransmission. [195][196][197][198][199][200] In addition, several lines of evidence have provided support for a role of Mecp2 in the regulation of activity-dependent transcription of Bdnf, 134,201,202 suggesting that alterations in 5-HT signaling could arise from deficient Mecp2 function, through dysregulation of Bdnf. Bdnf-null mice die soon after birth, but mutants have been developed with conditional disruption of Bdnf, limited to either the prenatal or postnatal period.…”

Section: Autism Candidate Genes and Synaptic Functionmentioning

confidence: 99%

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Advances in behavioral genetics: mouse models of autism

2007

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Autism is a neurodevelopmental syndrome with markedly high heritability. The diagnostic indicators of autism are core behavioral symptoms, rather than definitive neuropathological markers. Etiology is thought to involve complex, multigenic interactions and possible environmental contributions. In this review, we focus on genetic pathways with multiple members represented in autism candidate gene lists. Many of these pathways can also be impinged upon by environmental risk factors associated with the disorder. The mouse model system provides a method to experimentally manipulate candidate genes for autism susceptibility, and to use environmental challenges to drive aberrant gene expression and cell pathology early in development. Mouse models for fragile X syndrome, Rett syndrome and other disorders associated with autistic-like behavior have elucidated neuropathology that might underlie the autism phenotype, including abnormalities in synaptic plasticity. Mouse models have also been used to investigate the effects of alterations in signaling pathways on neuronal migration, neurotransmission and brain anatomy, relevant to findings in autistic populations. Advances have included the evaluation of mouse models with behavioral assays designed to reflect disease symptoms, including impaired social interaction, communication deficits and repetitive behaviors, and the symptom onset during the neonatal period. Research focusing on the effect of gene-by-gene interactions or genetic susceptibility to detrimental environmental challenges may further understanding of the complex etiology for autism.

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Increased BDNF Promoter Methylation in the Wernicke Area of Suicide Subjects

Keller¹,

Sarchiapone²,

Zarrilli³

et al. 2010

Arch Gen Psychiatry

347

217

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BDNF promoter/exon IV is frequently hypermethylated in the Wernicke area of the postmortem brain of suicide subjects irrespective of genome-wide methylation levels, indicating that a gene-specific increase in DNA methylation could cause or contribute to the downregulation of BDNF expression in suicide subjects. The reported data reveal a novel link between epigenetic alteration in the brain and suicidal behavior.

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Brain-Specific Phosphorylation of MeCP2 Regulates Activity-Dependent Bdnf Transcription, Dendritic Growth, and Spine Maturation

Cited by 762 publications

References 53 publications

The mood stabilizers lithium and valproate selectively activate the promoter IV of brain-derived neurotrophic factor in neurons

The mood stabilizers lithium and valproate selectively activate the promoter IV of brain-derived neurotrophic factor in neurons

Advances in behavioral genetics: mouse models of autism

Increased BDNF Promoter Methylation in the Wernicke Area of Suicide Subjects

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