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- Ando, Ryo1
- Ebina, Masayuki1
- Funayama, Ryo1
- Itoh-Nakadai, Ari1
- Kato, Hiroki1
- Katoh, Yasutake1
- Maeda, Tatsuya1
- Matsumoto, Mitsuyo1
- Motohashi, Hozumi1
- Muto, Akihiko1
- Nakayama, Keiko1
- Nio, Masaki1
- Ochiai, Kyoko1
- Sato, Masaki1
- Sax, Nicolas1
- Shima, Hiroki1
- Taguchi, Keiko1
- Tamahara, Toru1
- Unno, Michiaki1
- Watanabe-Matsui, Miki1
- Yamamoto, Masayuki1
Gene Regulation
2 Results
- Genomics and ProteomicsOpen Access
Regulatory signatures of liver regeneration distilled by integrative analysis of mRNA, histone methylation, and proteomics
Journal of Biological ChemistryVol. 292Issue 19p8019–8037Published online: March 16, 2017- Yoshihiro Sato
- Yasutake Katoh
- Mitsuyo Matsumoto
- Masaki Sato
- Masayuki Ebina
- Ari Itoh-Nakadai
- and others
Cited in Scopus: 12The capacity of the liver to regenerate is likely to be encoded as a plasticity of molecular networks within the liver. By applying a combination of comprehensive analyses of the epigenome, transcriptome, and proteome, we herein depict the molecular landscape of liver regeneration. We demonstrated that histone H3 Lys-4 was trimethylated at the promoter regions of many loci, among which only a fraction, including cell-cycle-related genes, were transcriptionally up-regulated. A cistrome analysis guided by the histone methylation patterns and the transcriptome identified FOXM1 as the key transcription factor promoting liver regeneration, which was confirmed in vitro using a hepatocarcinoma cell line. - Signal TransductionOpen Access
The Transcription Factor Bach2 Is Phosphorylated at Multiple Sites in Murine B Cells but a Single Site Prevents Its Nuclear Localization
Journal of Biological ChemistryVol. 291Issue 4p1826–1840Published online: November 30, 2015- Ryo Ando
- Hiroki Shima
- Toru Tamahara
- Yoshihiro Sato
- Miki Watanabe-Matsui
- Hiroki Kato
- and others
Cited in Scopus: 27The transcription factor Bach2 regulates the immune system at multiple points, including class switch recombination (CSR) in activated B cells and the function of T cells in part by restricting their terminal differentiation. However, the regulation of Bach2 expression and its activity in the immune cells are still unclear. Here, we demonstrated that Bach2 mRNA expression decreased in Pten-deficient primary B cells. Bach2 was phosphorylated in primary B cells, which was increased upon the activation of the B cell receptor by an anti-immunoglobulin M (IgM) antibody or CD40 ligand.