Suppression of MAGE-A10 alters the metastatic phenotype of tongue squamous cell carcinoma cells

Mendonça, Bruna dos Santos; Agostini, Michelle; Aquino, Iara Gonçalves; Dias, Wagner B.; Bastos, Débora Campanella; Rumjanek, Franklin David

doi:10.1016/j.bbrep.2017.04.009

Cited by 7 publications

(10 citation statements)

References 46 publications

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“…For example, MAGE proteins are known to be assembled with E3 RING ubiquitin alloys to form MAGE-RING alloys (MRLs) that function in many cell lines, including tumor cell proliferation (28) and total heat production. As shown in a previous paper (12), by silencing MAGEA10 in LN-1 and LN-2 cells, we observed a reduction as measured by migration and invasion. Indeed, by inhibiting the polymerization of the actin with cytochalasin D, we observed a smaller heat release, especially in the more aggressive cell line (Figure 3).…”

Section: Discussionsupporting

confidence: 88%

“…As we observed this increase in heat release exclusively in metastatic cell lines among the different tissues used (Figure 1), we decided to investigate what would be the interference, an increase of enthalpy, modulating MAGEA10, a protein closely related to the metastatic characteristics of tongue squamous carcinoma cells as shown in a paper by our group (12). Silencing this protein promotes a significant reduction in heat release (Figure 2), particularly in LN-2 cells.…”

Section: Discussionmentioning

confidence: 93%

“…Stable specific suppression of MAGEA10 mRNA was achieved by transduction of lentiviral particles expressing oligonucleotides bearing a short hairpin structure as described elsewhere (12).…”

Section: Suppression Of Human Magea10mentioning

confidence: 99%

“…Thus, we tested next whether the thermogenic differences observed in Figure 1 could be affected by the suppression of a protein that knowingly mediates adhesive properties of the LN cells. In a previous publication we have demonstrated that protein MAGEA10, which is highly expressed in metastatic cells, was involved in both, adhesion and motility of LN cells (12). Therefore, we carried out microcalorimetry experiments with LN cells stably suppressed for MAGEA10.…”

Section: Suppression Of Magea10 Reduces Heat Release By Tumor Cellsmentioning

confidence: 99%

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Isothermal Microcalorimetry of Tumor Cells: Enhanced Thermogenesis by Metastatic Cells

et al. 2019

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Tumor cells exhibit rewired metabolism. We carried out comparative analyses attempting to investigate whether metabolic reprograming could be measured by isothermal microcalorimetry. Intact metastatic cell lines of tongue cell carcinoma, human and murine melanoma, lung, and breast tumors consistently released more heat than nonmetastatic cells or cells displaying lower metastatic potential. In tongue squamous carcinoma cells mitochondrial enriched extract reproduced the heat release pattern of intact cells. Cytochalasin D, an actin filament inhibitor, and suppression of metastasis marker Melanoma associated gene 10 (MAGEA10) decreased heat release. Uncoupling protein 2 was highly expressed in metastatic cells, but not in non-metastatic cells. Carnitine palmitoyl transferase-1 inhibitor, Etomoxir strongly inhibited heat release by metastatic cells, thus linking lipid metabolism to thermogenesis. We propose that heat release may be a quantifiable trait of the metastatic process.

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Section: Discussionsupporting

confidence: 88%

Section: Discussionmentioning

confidence: 93%

“…Stable specific suppression of MAGEA10 mRNA was achieved by transduction of lentiviral particles expressing oligonucleotides bearing a short hairpin structure as described elsewhere (12).…”

Section: Suppression Of Human Magea10mentioning

confidence: 99%

Section: Suppression Of Magea10 Reduces Heat Release By Tumor Cellsmentioning

confidence: 99%

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Isothermal Microcalorimetry of Tumor Cells: Enhanced Thermogenesis by Metastatic Cells

et al. 2019

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“…Some studies have shown that these proteins may also be important for different aspects of tumor biology, such as for the development of metastasis [69][70][71]. Mendonça et al [72], when investigating the roles of MAGE-A10 in squamous cell carcinoma cell lines, demonstrated that this protein is indeed involved in the epithelial to mesenchymal transition (EMT). This relation should be explained by the interference with the elements of the cytoskeleton.…”

Section: On Immunotherapymentioning

confidence: 99%

pMHC Structural Comparisons as a Pivotal Element to Detect and Validate T-Cell Targets for Vaccine Development and Immunotherapy—A New Methodological Proposal

Vianna

Mendes

Bragatte

et al. 2019

Cells

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The search for epitopes that will effectively trigger an immune response remains the “El Dorado” for immunologists. The development of promising immunotherapeutic approaches requires the appropriate targets to elicit a proper immune response. Considering the high degree of HLA/TCR diversity, as well as the heterogeneity of viral and tumor proteins, this number will invariably be higher than ideal to test. It is known that the recognition of a peptide-MHC (pMHC) by the T-cell receptor is performed entirely in a structural fashion, where the atomic interactions of both structures, pMHC and TCR, dictate the fate of the process. However, epitopes with a similar composition of amino acids can produce dissimilar surfaces. Conversely, sequences with no conspicuous similarities can exhibit similar TCR interaction surfaces. In the last decade, our group developed a database and in silico structural methods to extract molecular fingerprints that trigger T-cell immune responses, mainly referring to physicochemical similarities, which could explain the immunogenic differences presented by different pMHC-I complexes. Here, we propose an immunoinformatic approach that considers a structural level of information, combined with an experimental technology that simulates the presentation of epitopes for a T cell, to improve vaccine production and immunotherapy efficacy.

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Anticancer properties of the fatty acid synthase inhibitor TVB-3166 on oral squamous cell carcinoma cell lines

Aquino

Bastos

Zelaya

et al. 2020

Archives of Oral Biology

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Suppression of MAGE-A10 alters the metastatic phenotype of tongue squamous cell carcinoma cells

Cited by 7 publications

References 46 publications

Isothermal Microcalorimetry of Tumor Cells: Enhanced Thermogenesis by Metastatic Cells

Isothermal Microcalorimetry of Tumor Cells: Enhanced Thermogenesis by Metastatic Cells

pMHC Structural Comparisons as a Pivotal Element to Detect and Validate T-Cell Targets for Vaccine Development and Immunotherapy—A New Methodological Proposal

Anticancer properties of the fatty acid synthase inhibitor TVB-3166 on oral squamous cell carcinoma cell lines

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