Stress-Specific Activation and Repression of Heat Shock Factors 1 and 2

doi:10.1128/MCB.21.21.7163-7171.2001

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Molecular and Cellular Biology, November 2001, p. 7163-7171, Vol. 21, No. 21
0270-7306/01/$04.00+0 DOI: 10.1128/MCB.21.21.7163-7171.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

Stress-Specific Activation and Repression of Heat Shock Factors 1 and 2

Anu Mathew, Sameer K. Mathur, Caroline Jolly, Susan G. Fox, Soojin Kim, and Richard I. Morimoto^*

Department of Biochemistry, Molecular Biology, and Cell Biology, Rice Institute for Biomedical Research, Northwestern University, Evanston, Illinois 60208

Received 8 March 2001/Returned for modification 27 April 2001/Accepted 30 July 2001

Vertebrate cells express a family of heat shock transcription factors (HSF1 to HSF4) that coordinate the inducible regulationof heat shock genes in response to diverse signals. HSF1 is potentand activated rapidly though transiently by heat shock, whereasHSF2 is a less active transcriptional regulator but can retainits DNA binding properties for extended periods. Consequently,the differential activation of HSF1 and HSF2 by various stressesmay be critical for cells to survive repeated and diverse stresschallenges and to provide a mechanism for more precise regulationof heat shock gene expression. Here we show, using a novel DNAbinding and detection assay, that HSF1 and HSF2 are coactivatedto different levels in response to a range of conditions thatcause cell stress. Above a low basal activity of both HSFs, heatshock preferentially activates HSF1, whereas the amino acid analogueazetidine or the proteasome inhibitor MG132 coactivates both HSFsto different levels and hemin preferentially induces HSF2. Unexpectedly,we also found that heat shock has dramatic adverse effects onHSF2 that lead to its reversible inactivation coincident withrelocalization from the nucleus. The reversible inactivation ofHSF2 is specific to heat shock and does not occur with other stressorsor in cells expressing high levels of heat shock proteins. Theseresults reveal that HSF2 activity is negatively regulated by heatand suggest a role for heat shock proteins in the positive regulationofHSF2.

^* Corresponding author. Mailing address: Department of Biochemistry, Molecular Biology, and Cell Biology, Rice Institute forBiomedical Research, Northwestern University, 2153 North CampusDr., Evanston, IL 60208. Phone: (847) 491-3340. Fax: (847) 491-4461.E-mail: r-morimoto{at}northwestern.edu.

Present address: IGEN International, Inc., Gaithersburg, MD20877.

Present address: DyOGen, INSERM U309, Institut A. Bonniot, Domaine de la Merci, 38706 La Tronche Cedex,France.

Molecular and Cellular Biology, November 2001, p. 7163-7171, Vol. 21, No. 21
0270-7306/01/$04.00+0 DOI: 10.1128/MCB.21.21.7163-7171.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

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