ER stress protection in cancer cells: the multifaceted role of the heat shock protein TRAP1

Matassa, Danilo Swann; Arzeni, Diana; Landriscina, Matteo; Esposito, Franca

doi:10.2478/ersc-2014-0003

Cited by 2 publications

(1 citation statement)

References 63 publications

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“…In addition, TRAP1-silenced colon carcinoma cells exhibited lack of clonogenic ability in vitro and tumor formation in mice xenografts [ 15 ], thus supporting the relevance of TRAP1 in early phases of colon carcinogenesis. It is also noteworthy that about 60% of human CRCs with high TRAP1 expression are characterized by the parallel upregulation of a network of proteins involved in several cell functions, critical for colon carcinogenesis [ 5 , 10 , 11 , 13 , 14 , 18 , 27 , 28 ]. Thus, it is intriguing to speculate that TRAP1 upregulation may represent an early mechanism used by colon cancer cells to adapt to unfavorable environmental conditions and, thus, activate a number of pathways responsible for malignant transformation and tumor progression.…”

Section: Discussionmentioning

confidence: 99%

TRAP1 protein signature predicts outcome in human metastatic colorectal carcinoma

et al. 2017

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TRAP1 is a HSP90 molecular chaperone upregulated in colorectal carcinomas and involved in control of intracellular signaling, cell cycle, apoptosis and drug resistance, stemness and bioenergetics through co-traslational regulation of a network of client proteins. Thus, the clinical significance of TRAP1 protein network was analyzed in human colorectal cancers. TRAP1 and/or its client proteins were quantified, by immunoblot analysis, in 60 surgical specimens of colorectal carcinomas at different stages and, by immunohistochemistry, in 9 colorectal adenomatous polyps, 11 in situ carcinomas and 55 metastatic colorectal tumors. TRAP1 is upregulated at the transition between low-and high-grade adenomas, in in situ carcinomas and in about 60% of human colorectal carcinomas, being downregulated only in a small cohort of tumors. The analysis of TCGA database showed that a subgroup of colorectal tumors is characterized by gain/loss of TRAP1 copy number, this correlating with its mRNA and protein expression. Interestingly, TRAP1 is co-expressed with the majority of its client proteins and hierarchical cluster analysis showed that the upregulation of TRAP1 and associated 6-protein signature (i.e., IF2α, eF1A, TBP7, MAD2, CDK1 and βCatenin) identifies a cohort of metastatic colorectal carcinomas with a significantly shorter overall survival (HR 5.4; 95% C.I. 1.1-26.6; p=0.037). Consistently, the prognostic relevance of TRAP1 was confirmed in a cohort of 55 metastatic colorectal tumors. Finally, TRAP1 positive expression and its prognostic value are more evident in left colon cancers. These data suggest that TRAP1 protein network may provide a prognostic signature in human metastatic colorectal carcinomas.

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Section: Discussionmentioning

confidence: 99%

TRAP1 protein signature predicts outcome in human metastatic colorectal carcinoma

et al. 2017

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Salivary proteins offer insights into keratinocyte death during aphthous stomatitis. A case-crossover study

Cofré-Leiva,

Camargo-Ayala,

Vergara-Pérez

et al. 2023

BMC Oral Health

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Background The death of oral keratinocytes is a crucial step in the emergence of recurrent aphthous stomatitis (RAS, also known as aphthae or aphthous ulcers). Since there are no experimental models available to research aphthous ulcers, little is understood about this process. We hypothesize that saliva can be a data bank of information that offers insights on epithelial damage. Methods In this case-crossover study, we assessed the salivary proteome of patients with RAS (n = 36) in the presence and absence of ulcers using discovery proteomics and bioinformatics. Additionally, we contrasted these patterns with those of healthy individuals (n = 31) who had no prior aphthous ulceration. Results Salivary proteome showed that during the ulcerative phase, controlled cell death was downregulated. Due to its ability to distinguish between individuals with and without ulcers, the ATF6B protein raises the possibility that endoplasmic reticulum (ER) stress is responsible for the damage that leads to the death of oral keratinocytes. The high abundance of TRAP1 and ERN1 matches with this biological discovery. The type of death is immunogenic, according to the functional data found in a cell death database. Conclusion We identified a cellular process that can lead to the death of oral keratinocytes in the etiopathogenesis process of RAS. Future studies should be conducted to identify what is responsible for the increase in ER stress signaling that would lead to an anti-cell death response.

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ER stress protection in cancer cells: the multifaceted role of the heat shock protein TRAP1

Cited by 2 publications

References 63 publications

TRAP1 protein signature predicts outcome in human metastatic colorectal carcinoma

TRAP1 protein signature predicts outcome in human metastatic colorectal carcinoma

Salivary proteins offer insights into keratinocyte death during aphthous stomatitis. A case-crossover study

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