HER2/ErbB2 activates HSF1 and thereby controls HSP90 clients including MIF in HER2-overexpressing breast cancer

Schulz, Ramona; Streller, Felix; Ah, Scheel; Rüschoff, Josef; Reinert, MC; Dobbelstein, Matthias; Nd, Marchenko; Um, Moll

doi:10.1038/cddis.2013.508

Cited by 81 publications

(84 citation statements)

References 59 publications

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“…Hsf1 þ/À Neu þ mice also showed reduced association of the Hsp90 client protein c-RAF with HSP90 and reduced levels of AKT-ERK1/2 signaling (16). Similar findings with respect to stabilization of Hsp90 client proteins by Her2/HSF1 axis came from a study where inhibition of Her2 signaling resulted in the inhibition of HSF1 activity (phosphorylation) and the destabilization of HSP90 clients including MIF (macrophage migration inhibitory factor) and AKT (17). Recent studies have demonstrated that overexpression of mutant p53 also activates EGFR/Her2, leading to enhanced PI3K and MAPK signaling, which results in the phosphorylation and activation of HSF1 (32).…”

Section: Ras-mapk and Mutant P53 Signaling In Tumorssupporting

confidence: 65%

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Heat Shock Factor 1 in Protein Homeostasis and Oncogenic Signal Integration

2015

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Heat shock factor 1 (HSF1) is a stress-inducible transcription factor and has been described as a multi-faceted modulator of tumorigenesis. Heat shock, accumulation of misfolded proteins, or malignant transformation promotes the activation and nuclear translocation of HSF1, where it binds to the promoters of heat shock proteins and an array of nonheat shock-regulated proteins to upregulate their transcription. These stress-responsive and tumor-promoting genes in turn alter the ability of tumor cells to respond to a variety of stresses and enable them to thrive in less than favorable growth conditions. Although a direct role for HSF1 in promoting mRNA transcription of tumor-promoting genes has been suggested, it appears that this property is context-and celltype dependent. Furthermore, recent studies have demonstrated a direct involvement of mTOR signaling in regulating HSF1-mediated transcription, thus establishing a direct link between protein translation and HSF1 activity. Interestingly, there is a growing understanding of the signaling pathways that are modulated by HSF1 in a variety of tumor types and the co-option of these survival pathways by HSF1 to promote tumorigenesis. This review will focus on the role of HSF1 in protein homeostasis and HSF1-mediated oncogenic signaling pathways that together promote tumorigenesis. Cancer Res; 75(6); 907-12. Ó2015 AACR.

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Section: Ras-mapk and Mutant P53 Signaling In Tumorssupporting

confidence: 65%

“…Experimental evidence suggests that loss of HSF1 results in the decreased stability of HSP90 client proteins (mostly kinases) and inhibits their downstream signaling (described in the more detail in the following sections; refs. 16,17).…”

Section: Hsf1 and Protein Homeostasismentioning

confidence: 99%

Heat Shock Factor 1 in Protein Homeostasis and Oncogenic Signal Integration

2015

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“…Downstream signaling pathways are activated upon ErbB2 receptor activation through either heterodimerization with ligand bound EGFR, ErbB3, or ErbB4 family receptors, or in presence of overexpression of ErbB2 due to gene ampliication, by ligand independent homodimerization [12]. The homo/heterodimerization promotes the receptor activation that in turn leads to tyrosine phosphorylation of the C-terminal residues.…”

Section: Molecular Mechanisms Of Erbb2 Activationmentioning

confidence: 99%

ErbB2 Receptor in Breast Cancer: Implications in Cancer Cell Migration, Invasion and Resistance to Targeted Therapy

Camacho-Leal¹,

Sciortino²,

Cabodi³

2017

Breast Cancer - From Biology to Medicine

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Overexpression of ErbB2 is found in several types of human carcinomas. In breast tumors, ErbB2 overexpression is detected in up to 20% of patients. Breast cancers in with ampliication of ErbB2 are characterized by rapid tumor growth, lower survival rate and increased disease progression. The molecular mechanisms underlying the oncogenic action of ErbB2 involve a complex signaling network that tightly regulates malignant cell migration and invasion and hence metastatic potential. Recent eforts have been made to identify gene expression signatures of ErbB2-positive invasive breast cancers that may represent important mediators of ErbB2-induced tumorigenesis and metastatic progression.In this chapter, we will discuss the canonical ErbB2 signaling pathways responsible for tumor growth and dissemination along with newly identiied mediators such as adaptor protein p130Cas and miRNAs. From a therapeutic point of view, the treatment with anti-ErbB2 monoclonal antibody trastuzumab has greatly improved the outcomes of patients with ErbB2 aggressive cancer. Nevertheless, de novo and acquired resistance to trastuzumab therapy still represent a major clinical problem. In the second part of the chapter, we will provide an overview of the mechanisms so far implicated in the onset of resistance to targeted therapy and of the new strategies to overcome resistance.

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“…Moreover, it was recently demonstrated in HER2-overexpressing breast cancer cells that HSF1 is constitutively phosphorylated and activated by the HER2-PI3K-AKT-mTOR signaling pathway and controls Hsp90 client proteins, including MIF (macrophage migration inhibitory factor, a tumor promoting protein) [25].…”

Section: Hsf1 Regulates Ldha Transcription and Stimulates Glycolysis mentioning

confidence: 99%

Roles of HSF1 and Heat Shock Proteins in Cancer

Ohtsuka

2016

Hyperthermic Oncology From Bench to Bedside

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Heat shock proteins (HSPs) that are induced by various stresses, such as heat, work to protect cells from detrimental environmental stresses as molecular chaperones. The expression of HSPs is regulated by a specific transcription factor HSF1 (heat shock factor 1). The HSF1-HSPs system has long been considered to have an endogenous cytoprotective function. It has recently been shown, however, that HSF1 and HSPs are essential for cancer cell development and progression, and the HSF1-HSPs system seems to be co-opted or hijacked by cancer cells for their own survival. In this review, recent progress in understanding the roles of HSF1 and HSPs in cancer is discussed.

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HER2/ErbB2 activates HSF1 and thereby controls HSP90 clients including MIF in HER2-overexpressing breast cancer

Cited by 81 publications

References 59 publications

Heat Shock Factor 1 in Protein Homeostasis and Oncogenic Signal Integration

Heat Shock Factor 1 in Protein Homeostasis and Oncogenic Signal Integration

ErbB2 Receptor in Breast Cancer: Implications in Cancer Cell Migration, Invasion and Resistance to Targeted Therapy

Roles of HSF1 and Heat Shock Proteins in Cancer

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