Multiple epigenetic maintenance factors implicated by the loss of Mll2 in mouse development

doi:10.1242/dev.02302

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Development ePress online publication date 15 Mar 2006
doi: 10.1242/dev.02302

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Research article

Multiple epigenetic maintenance factors implicated by the loss of Mll2 in mouse development

Stefan Glaser, Julia Schaft, Sandra Lubitz, Kristina Vintersten, Frank van der Hoeven, Katharina R. Tufteland, Rein Aasland, Konstantinos Anastassiadis, Siew-Lan Ang, and A. Francis Stewart^*
^* Author for correspondence (e-mail: stewart{at}biotec.tu-dresden.de)

Epigenesis is the process whereby the daughters of a dividingcell retain a chromatin state determined before cell division.The best-studied cases involve the inheritance of heterochromaticchromosomal domains, and little is known about specific generegulation by epigenetic mechanisms. Recent evidence shows thatepigenesis pivots on methylation of nucleosomes at histone 3lysines 4, 9 or 27. Bioinformatics indicates that mammals haveseveral enzymes for each of these methylations, including atleast six histone 3 lysine 4 methyltransferases. To look forevidence of gene-specific epigenetic regulation in mammaliandevelopment, we examined one of these six, Mll2, using a multipurposeallele in the mouse to ascertain the loss-of-function phenotype.Loss of Mll2 slowed growth, increased apoptosis and retardeddevelopment, leading to embryonic failure before E11.5. Usingchimera experiments, we demonstrated that Mll2 is cell-autonomouslyrequired. Evidence for gene-specific regulation was also observed.Although Mox1 and Hoxb1 expression patterns were correctly established,they were not maintained in the absence of Mll2, whereas Wnt1and Otx2 were. The Mll2 loss-of-function phenotype is differentfrom that of its sister gene Mll, and they regulate differentHox complex genes during ES cell differentiation. Therefore,these two closely related epigenetic factors play differentroles in development and maintain distinct gene expression patterns.This suggests that other epigenetic factors also regulate particularpatterns and that development entails networks of epigeneticspecificities.

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