TY - JOUR
T1 - Transcriptional response to stress in the dynamic chromatin environment of cycling and mitotic cells
AU - Vihervaara, Anniina
AU - Sergelius, Christian
AU - Vasara, Jenni
AU - Blom, Malin A H
AU - Elsing, Alexandra N
AU - Roos-Mattjus, Pia
AU - Sistonen, Lea
PY - 2013/9/3
Y1 - 2013/9/3
N2 - Heat shock factors (HSFs) are the master regulators of transcription under protein-damaging conditions, acting in an environment where the overall transcription is silenced. We determined the genomewide transcriptional program that is rapidly provoked by HSF1 and HSF2 under acute stress in human cells. Our results revealed the molecular mechanisms that maintain cellular homeostasis, including HSF1-driven induction of polyubiquitin genes, as well as HSF1- and HSF2-mediated expression patterns of cochaperones, transcriptional regulators, and signaling molecules. We characterized the genomewide transcriptional response to stress also in mitotic cells where the chromatin is tightly compacted. We found a radically limited binding and transactivating capacity of HSF1, leaving mitotic cells highly susceptible to proteotoxicity. In contrast, HSF2 occupied hundreds of loci in the mitotic cells and localized to the condensed chromatin also in meiosis. These results highlight the importance of the cell cycle phase in transcriptional responses and identify the specific mechanisms for HSF1 and HSF2 in transcriptional orchestration. Moreover, we propose that HSF2 is an epigenetic regulator directing transcription throughout cell cycle progression.
AB - Heat shock factors (HSFs) are the master regulators of transcription under protein-damaging conditions, acting in an environment where the overall transcription is silenced. We determined the genomewide transcriptional program that is rapidly provoked by HSF1 and HSF2 under acute stress in human cells. Our results revealed the molecular mechanisms that maintain cellular homeostasis, including HSF1-driven induction of polyubiquitin genes, as well as HSF1- and HSF2-mediated expression patterns of cochaperones, transcriptional regulators, and signaling molecules. We characterized the genomewide transcriptional response to stress also in mitotic cells where the chromatin is tightly compacted. We found a radically limited binding and transactivating capacity of HSF1, leaving mitotic cells highly susceptible to proteotoxicity. In contrast, HSF2 occupied hundreds of loci in the mitotic cells and localized to the condensed chromatin also in meiosis. These results highlight the importance of the cell cycle phase in transcriptional responses and identify the specific mechanisms for HSF1 and HSF2 in transcriptional orchestration. Moreover, we propose that HSF2 is an epigenetic regulator directing transcription throughout cell cycle progression.
KW - Binding Sites/genetics
KW - Blotting, Western
KW - Cell Cycle/genetics
KW - Chromatin/genetics
KW - DNA-Binding Proteins/genetics
KW - Gene Expression Regulation
KW - Heat Shock Transcription Factors
KW - Heat-Shock Proteins/genetics
KW - Heat-Shock Response/genetics
KW - Humans
KW - K562 Cells
KW - Male
KW - Mitosis/genetics
KW - Molecular Chaperones/genetics
KW - Polyubiquitin/genetics
KW - Promoter Regions, Genetic/genetics
KW - Protein Binding
KW - RNA Interference
KW - Reverse Transcriptase Polymerase Chain Reaction
KW - Transcription Factors/genetics
KW - Transcription, Genetic
KW - Transcriptional Activation
U2 - 10.1073/pnas.1305275110
DO - 10.1073/pnas.1305275110
M3 - Article
C2 - 23959860
SN - 0027-8424
VL - 110
SP - E3388-97
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 36
ER -