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Crosstalk between histone modifications maintains the developmental pattern of gene expression on a tissue-specific locus

Pages 273-281 | Received 15 Feb 2010, Accepted 16 Feb 2010, Published online: 16 May 2010
 

Abstract

Genome wide studies have provided a wealth of information related to histone modifications. Particular modifications, which can encompass both broad and discrete regions, are associated with certain genomic elements and gene expression status. Here we focus on how studies on the ß-globin gene cluster can complement the genome wide effort through the thorough dissection of histone modifying protein crosstalk. The ß-globin locus serves as a model system to study both regulation of gene expression driven at a distance by enhancers and mechanisms of developmental switching of clustered genes. We investigate recent studies, which uncover that histone methyltransferases, recruited at the ß-globin enhancer, control gene expression by long range propagation on chromatin. Specifically, we focus on how seemingly antagonistic complexes, such as those including MLL2, G9a and UTX, can cooperate to functionally regulate developmentally controlled gene expression. Finally, we speculate on the mechanisms of chromatin modifying complex propagation on genomic domains.