TRAP1 enhances Warburg metabolism through modulation of PFK1 expression/activity and favors resistance to EGFR inhibitors in human colorectal carcinomas

Maddalena, Francesca; Condelli, Valentina; Matassa, Danilo Swann; Pacelli, Consiglia; Scrima, Rosella; Lettini, Giacomo; Bergolis, Valeria Li; Pietrafesa, Michele; Crispo, Fabiana; Piscazzi, Annamaria; Storto, Giovanni; Capitanio, Nazzareno; Esposito, Franca; Landriscina, Matteo

doi:10.1002/1878-0261.12814

Cited by 24 publications

(23 citation statements)

References 52 publications

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“…Our data suggested that C501 oxidation is a mediator of AF toxicity, and we found that C501S mutation decreased the cell sensitivity to AF treatment. As previously reported, TRAP1 C501 S -nitrosylation impacts its protein expression levels and ATPase activity, both important for TRAP1 role in regulating the Warburg effect and sensitivity to drugs [ 63 , 64 , 98 , 99 ]. Here, the observed decreased sensitivity of the TRAP1 C501S mutant to AF agrees with the effects of C501 S -nitrosylation shown in previous studies.…”

Section: Discussionmentioning

confidence: 87%

Redox proteome analysis of auranofin exposed ovarian cancer cells (A2780)

et al. 2022

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Section: Discussionmentioning

confidence: 87%

Redox proteome analysis of auranofin exposed ovarian cancer cells (A2780)

et al. 2022

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“…The effects of TRAP1 on mitochondrial respiration are still controversial: TRAP1 silencing increases oxygen consumption in SAOS-2 osteosarcoma cells, PEA1 ovarian cancer cells, HCT116 colorectal carcinoma cells and mouse fibroblasts [ 7 , 8 , 17 , 18 ]; however, TRAP1 silencing or treatment with the mitochondria-directed HSP90 inhibitor Gamitrinibs reduces oxygen consumption and ATP production in PC3 prostate cancer cells and in LN229 glioblastoma cells, although in the specific metabolic context of low glucose availability [ 9 ]. To shed light on this complex scenario, as a preliminary approach we first analyzed the response of TRAP1 knock-down cells to a decreased glucose availability through the monitoring of AMPK activation over time and identified a significant AMPK phosphorylation after 4 h of glucose withdrawal (referred to as "low glucose” hereafter), specifically in TRAP1-expressing cells (Additional file 1 : Fig.…”

Section: Resultsmentioning

confidence: 99%

Regulation of mitochondrial complex III activity and assembly by TRAP1 in cancer cells

et al. 2022

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Background Metabolic reprogramming is an important issue in tumor biology. A recently-identified actor in this regard is the molecular chaperone TRAP1, that is considered an oncogene in several cancers for its high expression but an oncosuppressor in others with predominant oxidative metabolism. TRAP1 is mainly localized in mitochondria, where it interacts with respiratory complexes, although alternative localizations have been described, particularly on the endoplasmic reticulum, where it interacts with the translational machinery with relevant roles in protein synthesis regulation. Results Herein we show that, inside mitochondria, TRAP1 binds the complex III core component UQCRC2 and regulates complex III activity. This decreases respiration rate during basal conditions but allows sustained oxidative phosphorylation when glucose is limiting, a condition in which the direct TRAP1-UQCRC2 binding is disrupted, but not TRAP1-complex III binding. Interestingly, several complex III components and assembly factors show an inverse correlation with survival and response to platinum-based therapy in high grade serous ovarian cancers, where TRAP1 inversely correlates with stage and grade and directly correlates with survival. Accordingly, drug-resistant ovarian cancer cells show high levels of complex III components and high sensitivity to complex III inhibitory drug antimycin A. Conclusions These results shed new light on the molecular mechanisms involved in TRAP1-dependent regulation of cancer cell metabolism and point out a potential novel target for metabolic therapy in ovarian cancer.

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“…However, male sterility due to malfunction of the MMI system is indeed a loss for species preservation, and it seems that some kind of defense system coexists. Fmr1 is involved in spermatogenesis, axoneme synthesis, and the Warburg effect (Zhang et al, 2004;Maddalena et al, 2020), and its function is very similar to that of SPAG1, so it may control SPAG1-2 expression as an RNA-binding translational regulatory protein. If the SPAG1-2 / Eri15 axis runs out of control due to widespread loss of Fx-mir, it may be that the misexpressed FMRP suppresses the translation of SPAG1-2 mRNA.…”

Section: Xt-mir and Spag1mentioning

confidence: 99%

On The Origin of Speciation

Hayashida¹

2022

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Charles Darwin proposed the theory of evolution that natural selection leads to the evolution of organisms in "On the Origin of Species”, but did not show the mechanism by which new species differentiate and fix. Speciation requires a system in which genes are not mixed by interspecific hybridization, and reproductive isolation, especially postmating reproductive isolation, is considered to be the most reliable as guarantee. Haldane proposed that heterogametic sex was absent, rare or sterile in interspecific hybrid F1. Dobzhansky and Muller predicted that postmating reproductive isolation occurs when mutations occurring at two or more interacting loci exhibit incompatibility in the hybrid. Genes that satisfy these observation and prediction are considered speciation genes. Here, I would like to review the findings on reproductive isolation and speciation to consider the candidate conditions for the speciation genes, and present the genes that fit these conditions.

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TRAP1 enhances Warburg metabolism through modulation of PFK1 expression/activity and favors resistance to EGFR inhibitors in human colorectal carcinomas

Cited by 24 publications

References 52 publications

Redox proteome analysis of auranofin exposed ovarian cancer cells (A2780)

Redox proteome analysis of auranofin exposed ovarian cancer cells (A2780)

Regulation of mitochondrial complex III activity and assembly by TRAP1 in cancer cells

On The Origin of Speciation

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