| Literature DB >> 31940498 |
Jenny Joutsen1, Alejandro Jose Da Silva1, Jens Christian Luoto1, Marek Andrzej Budzynski1, Anna Serafia Nylund1, Aurelie de Thonel2, Jean-Paul Concordet3, Valérie Mezger2, Délara Sabéran-Djoneidi2, Eva Henriksson1, Lea Sistonen4.
Abstract
Maintenance of protein homeostasis, through inducible expression of molecular chaperones, is essential for cell survival under protein-damaging conditions. The expression and DNA-binding activity of heat shock factor 2 (HSF2), a member of the heat shock transcription factor family, increase upon exposure to prolonged proteotoxicity. Nevertheless, the specific roles of HSF2 and the global HSF2-dependent gene expression profile during sustained stress have remained unknown. Here, we found that HSF2 is critical for cell survival during prolonged proteotoxicity. Strikingly, our RNA sequencing (RNA-seq) analyses revealed that impaired viability of HSF2-deficient cells is not caused by inadequate induction of molecular chaperones but is due to marked downregulation of cadherin superfamily genes. We demonstrate that HSF2-dependent maintenance of cadherin-mediated cell-cell adhesion is required for protection against stress induced by proteasome inhibition. This study identifies HSF2 as a key regulator of cadherin superfamily genes and defines cell-cell adhesion as a determinant of proteotoxic stress resistance.Entities:
Keywords: Bortezomib; cadherins; cell adhesion; cell survival; heat shock factor; proteotoxic stress
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Year: 2020 PMID: 31940498 DOI: 10.1016/j.celrep.2019.12.037
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423