Genome-Wide Screening for Target Regions of Histone Deacetylases in Cardiomyocytes

doi:10.1161/01.RES.0000176028.18423.07

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Circulation Research. 2005;97:210-218
Published online before print July 7, 2005, doi: 10.1161/01.RES.0000176028.18423.07

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(Circulation Research. 2005;97:210.)
© 2005 American Heart Association, Inc.

Molecular Medicine

Genome-Wide Screening for Target Regions of Histone Deacetylases in Cardiomyocytes

Ruri Kaneda, Shuichi Ueno, Yoshihiro Yamashita, Young Lim Choi, Koji Koinuma, Shuji Takada, Tomoaki Wada, Kazuyuki Shimada, Hiroyuki Mano

From the Divisions of Functional Genomics (R.K., S.U., Y.Y., Y.L.C., K.K., S.T., T.W., H.M.) and Cardiovascular Medicine (R.K., S.U., K.S.), Jichi Medical School, Tochigi, Japan; and CREST (H.M.), Japan Science and Technology Agency, Saitama.

Correspondence to Dr Hiroyuki Mano, Division of Functional Genomics, Jichi Medical School, 3311-1 Yakushiji, Kawachigun, Tochigi 329-0498, Japan. E-mail hmano{at}jichi.ac.jp

The acetylation status of core histones in cardiomyocytes hasbeen linked to the development of cardiac hypertrophy and heartfailure. Little is known, however, of the genes affected byabnormal histone acetylation in such pathological conditions.We recently developed a genome-wide screening method, differentialchromatin scanning (DCS), to isolate genomic fragments associatedwith histones subject to differential acetylation. We have nowapplied DCS to H9C2 rat embryonic cardiomyocytes incubated withor without trichostatin A (TSA), a specific inhibitor of histonedeacetylase (HDAC) activity. About 200 genomic fragments werereadily isolated by DCS on the basis of the preferential acetylationof associated histones in TSA-treated cells. Quantitation ofthe amount of DNA in chromatin immunoprecipitates prepared withantibodies to acetylated histone H3 revealed that 37 of 38 randomlychosen DCS clones were preferentially precipitated from theTSA-treated cells, thus verifying the high fidelity of DCS.Epigenetic regulation of DCS clones was further confirmed incells treated with sodium butyrate, another HDAC inhibitor,as well as in cardiac myocytes isolated from neonatal rats.The mRNA level of 9 (39%) of 23 genes corresponding to DCS cloneschanged in parallel with the level of histone acetylation inH9C2 cells. Furthermore, a physiological hypertrophic stimulus,cardiotrophin-1, affected the acetylation level of histonesassociated with genomic regions corresponding to certain DCSclones. Our data thus establish a genome-wide profile of HDACtargets in cardiomyocytes, which should provide a basis forfurther investigations into the role of epigenetic modificationin cardiac disorders.

Key Words: epigenetics • histone acetylation • trichostatin A • cardiomyocyte

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