DNA hypomethylation restricted to the murine forebrain induces cortical degeneration and impairs postnatal neuronal maturation

doi:10.1093/hmg/ddp222

Human Molecular Genetics Advance Access originally published online on May 10, 2009
Human Molecular Genetics 2009 18(15):2875-2888; doi:10.1093/hmg/ddp222

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DNA hypomethylation restricted to the murine forebrain induces cortical degeneration and impairs postnatal neuronal maturation

Leah K. Hutnick¹^,2, Peyman Golshani³^,4, Masakasu Namihira¹, Zhigang Xue¹, Anna Matynia³, X. William Yang⁵, Alcino J. Silva³^,5^,6, Felix E. Schweizer³ and Guoping Fan¹^,2^,*

¹ Department of Human Genetics ² Department of Neuroscience Interdepartmental Program, David Geffen School of Medicine, University of California at Los Angeles, 695 Charles Young Drive South, Los Angeles, CA 90095, USA ³ Department of Neurobiology ⁴ Department of Neurology ⁵ Department of Psychiatry and Behavioral Sciences ⁶ Department of Psychology, UCLA, Los Angeles, CA 90095, USA

^* To whom correspondence should be addressed. Tel: +1 3102670439; Fax: +1 3107945446; Email: gfan{at}mednet.ucla.edu

Received February 27, 2009; Revised April 18, 2009; Accepted May 6, 2009

DNA methylation is a major epigenetic factor regulating genomereprogramming, cell differentiation and developmental gene expression.To understand the role of DNA methylation in central nervoussystem (CNS) neurons, we generated conditional Dnmt1 mutantmice that possess $~$ 90% hypomethylated cortical and hippocampalcells in the dorsal forebrain from E13.5 on. The mutant micewere viable with a normal lifespan, but displayed severe neuronalcell death between E14.5 and three weeks postnatally. Accompaniedwith the striking cortical and hippocampal degeneration, adultmutant mice exhibited neurobehavioral defects in learning andmemory in adulthood. Unexpectedly, a fraction of Dnmt1^–/–cortical neurons survived throughout postnatal development,so that the residual cortex in mutant mice contained 20–30%of hypomethylated neurons across the lifespan. Hypomethylatedexcitatory neurons exhibited multiple defects in postnatal maturationincluding abnormal dendritic arborization and impaired neuronalexcitability. The mutant phenotypes are coupled with deregulationof those genes involved in neuronal layer-specification, celldeath and the function of ion channels. Our results suggestthat DNA methylation, through its role in modulating neuronalgene expression, plays multiple roles in regulating cell survivaland neuronal maturation in the CNS.

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