Cells (Apr 2020)

HSF1: Primary Factor in Molecular Chaperone Expression and a Major Contributor to Cancer Morbidity

  • Thomas L. Prince,
  • Benjamin J. Lang,
  • Martin E. Guerrero-Gimenez,
  • Juan Manuel Fernandez-Muñoz,
  • Andrew Ackerman,
  • Stuart K. Calderwood

DOI
https://doi.org/10.3390/cells9041046
Journal volume & issue
Vol. 9, no. 4
p. 1046

Abstract

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Heat shock factor 1 (HSF1) is the primary component for initiation of the powerful heat shock response (HSR) in eukaryotes. The HSR is an evolutionarily conserved mechanism for responding to proteotoxic stress and involves the rapid expression of heat shock protein (HSP) molecular chaperones that promote cell viability by facilitating proteostasis. HSF1 activity is amplified in many tumor contexts in a manner that resembles a chronic state of stress, characterized by high levels of HSP gene expression as well as HSF1-mediated non-HSP gene regulation. HSF1 and its gene targets are essential for tumorigenesis across several experimental tumor models, and facilitate metastatic and resistant properties within cancer cells. Recent studies have suggested the significant potential of HSF1 as a therapeutic target and have motivated research efforts to understand the mechanisms of HSF1 regulation and develop methods for pharmacological intervention. We review what is currently known regarding the contribution of HSF1 activity to cancer pathology, its regulation and expression across human cancers, and strategies to target HSF1 for cancer therapy.

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