Fission yeast global repressors regulate the specificity of chromatin alteration in response to distinct environmental stresses

doi:10.1093/nar/gkh251

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Published online 3 February 2004

Nucleic Acids Research, 2004, Vol. 32, No. 2 855-862
© 2004 Oxford University Press

Fission yeast global repressors regulate the specificity of chromatin alteration in response to distinct environmental stresses

Kouji Hirota¹, Tomoko Hasemi¹, Takatomi Yamada¹, Ken-ich Mizuno¹, Charles S. Hoffman², Takehiko Shibata³ and Kunihiro Ohta^*^,1^,3

¹ Genetic Dynamics Research Unit-Laboratory, RIKEN (Institute of Physical and Chemical Research), Wako-shi, Saitama 351-0198, Japan, ² Biology Department, Boston College, Chestnut Hill, MA 02467 USA and ³ Cellular and Molecular Biology Laboratory, RIKEN (Institute of Physical and Chemical Research)/CREST of the JST, Wako-shi, Saitama 351-0198, Japan

*To whom correspondence should be addressed at Genetic Dynamics Research Unit-Laboratory, RIKEN (The Institute of Physical and Chemical Research), Wako-shi, Saitama 351-0198, Japan. Tel: +81 48 467 9538; Fax: +81 48 462 4671; Email: kohta{at}postman.riken.go.jp

The specific induction of genes in response to distinct environmentalstress is vital for all eukaryotes. To study the mechanismsthat result in selective gene responses, we examined the roleof the fission yeast Tup1 family repressors in chromatin regulation.We found that chromatin structure around a cAMP-responsive element(CRE)-like sequence in ade6-M26 that is bound by Atf1·Pcr1transcriptional activation was altered in response to osmoticstress but not to heat and oxidative stresses. Such chromatinstructure alteration occurred later than the Atf1 phosphorylationbut correlated well with stress-induced transcriptional activationat ade6-M26. This chromatin structure alteration required componentsfor the stress-activated protein kinase (SAPK) cascade and bothsubunits of the M26-binding CREB/ATF-type protein Atf1·Pcr1.Cation stress and glucose starvation selectively caused chromatinstructure alteration around CRE-like sequences in cta3⁺ andfbp1⁺ promoters, respectively, in correlation with transcriptionalactivation. However, the tup11 ${Delta}$ tup12 ${Delta}$ double deletion mutantslost the selectivity of stress responses of chromatin structureand transcriptional regulation of cta3⁺ and fbp1⁺. These dataindicate that the Tup1-like repressors regulate the chromatinstructure to ensure the specificity of gene activation in responseto particular stresses. Such a role for these proteins may serveas a paradigm for the regulation of stress response in highereukaryotes.

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