Hsp-27 induction requires POU4F2/Brn-3b TF in doxorubicin-treated breast cancer cells, whereas phosphorylation alters its cellular localisation following drug treatment

Fujita, Rieko; Ounzain, Samir; Wang, Alice Chun Yin; Heads, Richard J.; Budhram-Mahadeo, Vishwanie

doi:10.1007/s12192-011-0256-8

Cited by 17 publications

(17 citation statements)

References 53 publications

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“…Both Hsp27 and Hsp70 (and other HSPs) can block apoptosis therefore it is complicated to maintain the fine tuning in HSP expression levels to allow the drugs to effectively kill cancer cells. In line with this, Fujita et al (2011) reported in MCF-7 cells that survived to doxorubicin that the POU4F2/Brn-3b transcription factor is increased with concomitant increases in Hsp27 expression. The POU4F2/Brn-3b transcription factor is required to maximally trans -activate Hsp27 and is elevated in >60% of breast cancers altering growth and behavior of cancer cells by regulating distinct subsets of target genes.…”

Section: Introductionsupporting

confidence: 67%

Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: an update

2012

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Heat shock proteins (HSP) are a subset of the molecular chaperones, best known for their rapid and abundant induction by stress. HSP genes are activated at the transcriptional level by heat shock transcription factor 1 (HSF1). During the progression of many types of cancer, this heat shock transcriptional regulon becomes co-opted by mechanisms that are currently unclear, although evidently triggered in the emerging tumor cell. Concerted activation of HSF1 and the accumulation of HSPs then participates in many of the traits that permit the malignant phenotype. Thus cancers of many histologies exhibit activated HSF1 and increased HSP levels that may help to deter tumor suppression and evade therapy in the clinic. We review here the extensive work that has been carried out and is still in progress aimed at: (1) understanding the oncogenic mechanisms by which HSP genes are switched on, (2) determining the roles of HSF1 / HSP in malignant transformation and, (3) discovering approaches to therapy based on disrupting the influence of the HSF1 controlled transcriptome in cancer.

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Section: Introductionsupporting

confidence: 67%

Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: an update

2012

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“…In breast cancer, POU4F2 can repress BRCA1 expression [36] and interact with estrogen receptor alpha to enhance its activity [35]. POU4F2 can also induce the expression of CCD1 and CDK4 in the context of proliferation and cell cycle progression [34,37], confer migratory and multidrug resistance properties to breast cancer in in vivo models [38], and cooperate with TP53 to increase transcription of pro-apoptotic genes [39]. Importantly, growth factors like the epidermal growth factor (EGF) can stimulate the activity of the POU4F2 promoter and subsequently its mRNA and protein expression, which in turn can affect POU4F2 target genes influencing growth and behavior of cancer cells.…”

Section: Discussionmentioning

confidence: 99%

Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study

et al. 2016

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BackgroundLung adenocarcinoma (LUAD) is the most common histologic subtype of lung cancer and has a high risk of distant metastasis at every disease stage. We aimed to characterize the genomic landscape of LUAD and identify mutation signatures associated with tumor progression.Methods and FindingsWe performed an integrative genomic analysis, incorporating whole exome sequencing (WES), determination of DNA copy number and DNA methylation, and transcriptome sequencing for 101 LUAD samples from the Environment And Genetics in Lung cancer Etiology (EAGLE) study. We detected driver genes by testing whether the nonsynonymous mutation rate was significantly higher than the background mutation rate and replicated our findings in public datasets with 724 samples. We performed subclonality analysis for mutations based on mutant allele data and copy number alteration data. We also tested the association between mutation signatures and clinical outcomes, including distant metastasis, survival, and tumor grade. We identified and replicated two novel candidate driver genes, POU class 4 homeobox 2 (POU4F2) (mutated in 9 [8.9%] samples) and ZKSCAN1 (mutated in 6 [5.9%] samples), and characterized their major deleterious mutations. ZKSCAN1 was part of a mutually exclusive gene set that included the RTK/RAS/RAF pathway genes BRAF, EGFR, KRAS, MET, and NF1, indicating an important driver role for this gene. Moreover, we observed strong associations between methylation in specific genomic regions and somatic mutation patterns. In the tumor evolution analysis, four driver genes had a significantly lower fraction of subclonal mutations (FSM), including TP53 (p = 0.007), KEAP1 (p = 0.012), STK11 (p = 0.0076), and EGFR (p = 0.0078), suggesting a tumor initiation role for these genes. Subclonal mutations were significantly enriched in APOBEC-related signatures (p < 2.5×10−50). The total number of somatic mutations (p = 0.0039) and the fraction of transitions (p = 5.5×10−4) were associated with increased risk of distant metastasis. Our study’s limitations include a small number of LUAD patients for subgroup analyses and a single-sample design for investigation of subclonality.ConclusionsThese data provide a genomic characterization of LUAD pathogenesis and progression. The distinct clonal and subclonal mutation signatures suggest possible diverse carcinogenesis pathways for endogenous and exogenous exposures, and may serve as a foundation for more effective treatments for this lethal disease. LUAD’s high heterogeneity emphasizes the need to further study this tumor type and to associate genomic findings with clinical outcomes.

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“…or higher Electronic supplementary material The online version of this article (doi:10.1007/s12192-015-0662-4) contains supplementary material, which is available to authorized users. eukaryotes (Adamska and Kloppstech 1991;Eisenberg-Domovich et al 1994;Heckathorn et al 1998;Bausero et al 2005;de Miguel et al 2008;Fujita et al 2011). Whether different Hsps interact only with membrane proteins, only with membrane lipids, or with both remains to be explored.…”

Section: Introductionmentioning

confidence: 99%

Involvement of small heat shock proteins, trehalose, and lipids in the thermal stress management in Schizosaccharomyces pombe

Glatz

Pilbat

Németh

et al. 2016

Cell Stress and Chaperones

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Changes in the levels of three structurally and functionally different important thermoprotectant molecules, namely small heat shock proteins (sHsps), trehalose, and lipids, have been investigated upon heat shock in Schizosaccharomyces pombe. Both α-crystallin-type sHsps (Hsp15.8 and Hsp16) were induced after prolonged high-temperature treatment but with different kinetic profiles. The shsp null mutants display a weak, but significant, heat sensitivity indicating their importance in the thermal stress management. The heat induction of sHsps is different in wild type and in highly heat-sensitive trehalose-deficient (tps1Δ) cells; however, trehalose level did not show significant alteration in shsp mutants. The altered timing of trehalose accumulation and induction of sHsps suggest that the disaccharide might provide protection at the early stage of the heat stress while elevated amount of sHsps are required at the later phase. The cellular lipid compositions of two different temperature-adapted wild-type S. pombe cells are also altered according to the rule of homeoviscous adaptation, indicating their crucial role in adapting to the environmental temperature changes. Both Hsp15.8 and Hsp16 are able to bind to different lipids isolated from S. pombe, whose interaction might provide a powerful protection against heat-induced damages of the membranes. Our data suggest that all the three investigated thermoprotectant macromolecules play a pivotal role during the thermal stress management in the fission yeast.

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Hsp-27 induction requires POU4F2/Brn-3b TF in doxorubicin-treated breast cancer cells, whereas phosphorylation alters its cellular localisation following drug treatment

Cited by 17 publications

References 53 publications

Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: an update

Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: an update

Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study

Involvement of small heat shock proteins, trehalose, and lipids in the thermal stress management in Schizosaccharomyces pombe

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