Chromosome-wide, allele-specific analysis of the histone code on the human X chromosome

doi:10.1093/hmg/ddl159

Human Molecular Genetics Advance Access originally published online on June 20, 2006
Human Molecular Genetics 2006 15(15):2335-2347; doi:10.1093/hmg/ddl159

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Chromosome-wide, allele-specific analysis of the histone code on the human X chromosome

Cory M. Valley¹^,2, Lisa M. Pertz¹, Bala S. Balakumaran¹ and Huntington F. Willard¹^,2^,3^,*

¹ Institute for Genome Sciences & Policy, ² Department of Molecular Genetics and Microbiology and ³ Department of Biology, Duke University, Durham, NC 27708, USA

^* To whom correspondence should be addressed at: Institute for Genome Sciences & Policy, Duke University, CIEMAS 2376, 101 Science Drive, Durham, NC 27708, USA. Tel: +1 9196684477; Fax: +1 9196680795; Email: hunt.willard{at}duke.edu

Received March 7, 2006; Accepted June 16, 2006

Variation in the composition of chromatin has been proposedto generate a ‘histone code’ that epigeneticallyregulates gene expression in a variety of eukaryotic systems.As a result of the process of X chromosome inactivation, chromatinonthe mammalian inactive X chromosome (Xi) is marked by severalmodifications, including histone hypoacetylation, trimethylationof lysine 9 on histone H3 (H3TrimK9) and substitution of corehistone H2A with the histone variant MacroH2A. H3TrimK9 is awell-studied marker for heterochromatin in many organisms, butthe distribution and function of MacroH2A are less clear. Cytologically,the Xi in human cells comprises alternating and largely non-overlapping $~$ 10–15 Mb domains marked by MacroH2A and H3TrimK9.To examine the genomic deposition of MacroH2A, H3TrimK9 andacetylated histone H4 modifications on the Xi at higher resolution,we used chromatin immunoprecipitation in combination with aSNP-based assay to distinguish the Xi and active X (Xa) in adiploid female cell line and to determine quantitatively therelative enrichment of these histone code elements on the Xirelative to the Xa. Although we found a majority of sites wereenriched for either MacroH2A or H3TrimK9 in a manner consistentwith the cytological appearance of the Xi, a range of differenthistone code types were detected at different sites along theX. These findings suggest that the nature of the heterochromatinhistone code associated with X inactivation may be more heterogeneousthan previously thought and imply that gene silencing can beachieved by a variety of different epigenetic mechanisms whosegenomic, evolutionary or developmental basis is now amenableto investigation.

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