Bcl-2-like protein-10 increases aggressive features of melanoma cells

Del Bufalo, Donatella; Di Martile, Marta; Valentini, Elisabetta; Manni, Isabella; Masi, Ilenia; D'Amore, Antonella; Filippini, Antonio; Nicoletti, Carmine; Zaccarini, Marco; Cota, Carlo; Castro, María Victoria; Quezada, Maria Josefina; Rosanò, Laura; Lopez Bergami, Pablo Roberto; D'Aguanno, Simona

doi:10.37349/etat.2022.00068

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dc.contributor.author

Del Bufalo, Donatella

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Di Martile, Marta

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Valentini, Elisabetta

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Manni, Isabella

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Masi, Ilenia

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D'Amore, Antonella

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Filippini, Antonio

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Nicoletti, Carmine

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Zaccarini, Marco

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Cota, Carlo

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Castro, María Victoria Se ha confirmado la validez de este valor de autoridad por un usuario

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Quezada, Maria Josefina Se ha confirmado la validez de este valor de autoridad por un usuario

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Rosanò, Laura

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Lopez Bergami, Pablo Roberto Se ha confirmado la validez de este valor de autoridad por un usuario

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D'Aguanno, Simona

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2022-07-07T12:58:28Z

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2022-01

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Del Bufalo, Donatella; Di Martile, Marta; Valentini, Elisabetta; Manni, Isabella; Masi, Ilenia; et al.; Bcl-2-like protein-10 increases aggressive features of melanoma cells; Open Exploration; Exploration of Targeted Anti-tumor Therapy; 3; 1-2022; 11-26

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http://hdl.handle.net/11336/161541

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Aim: B-cell lymphoma-2 (Bcl-2)-like protein-10 (Bcl2L10) is the less studied member of Bcl-2 family proteins, with the controversial role in different cancer histotypes. Very recently, Bcl2L10 expression in melanoma tumor specimens and its role in melanoma response to therapy have been demonstrated. Here, the involvement of Bcl2L10 on the in vitro and in vivo properties associated with melanoma aggressive features has been investigated. Methods: Endogenous Bcl2L10 protein expression was detected by western blotting analysis in a panel of patient-derived and commercially available human melanoma cells. In vitro assays to evaluate clonogenicity, cell proliferation, cell migration, cell invasion, and in vitro capillary-like structure formation [vasculogenic mimicry (VM)] have been performed by using human melanoma cells stably overexpressing Bcl2L10 or transiently transfected for loss/gain function of Bcl2L10, grown under two- or three-dimensional (3D) conditions Xenograft melanoma model was employed to evaluate in vivo tumor growth and angiogenesis. Results: Results demonstrated that Bcl2L10 acts as an inducer of in vitro cell migration, invasion, and VM, while in vitro cell proliferation, in vivo tumor growth, as well as colony formation properties were not affected. Dissecting different signaling pathways, it was found that Bcl2L10 positively affects the phosphorylation of extracellular-signal-regulated kinase (ERK) and the expression of markers of cell invasion, such as urokinase plasminogen activator receptor (uPAR) and matrix metalloproteinases (MMPs). Of note, Bcl2L10-dependent in vitro migration, invasion, and VM are linked to uPAR. Bcl2L10 also negatively regulates the intracellular calcium level. Finally, reduced invasion capability in 3D spheroid invasion assay of melanoma cells transiently overexpressing Bcl2L10 was observed after treatment with inhibitors of MMPs and uPAR. Conclusions: Overall, data reported in this paper provide evidence supporting a positive role of Bcl2L10 in melanoma aggressive features.

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application/pdf

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eng

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Open Exploration

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info:eu-repo/semantics/openAccess

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https://creativecommons.org/licenses/by/2.5/ar/

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B-cell lymphoma-2-like protein-10

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Melanoma

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Invasion

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Migration

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Vasculogenic mimicry

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Bioquímica y Biología Molecular Se ha confirmado la validez de este valor de autoridad por un usuario

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Ciencias Biológicas Se ha confirmado la validez de este valor de autoridad por un usuario

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CIENCIAS NATURALES Y EXACTAS Se ha confirmado la validez de este valor de autoridad por un usuario

dc.title

Bcl-2-like protein-10 increases aggressive features of melanoma cells

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info:eu-repo/semantics/article

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info:ar-repo/semantics/artículo

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info:eu-repo/semantics/publishedVersion

dc.date.updated

2022-06-30T19:02:20Z

dc.identifier.eissn

2692-3114

dc.journal.volume

3

dc.journal.pagination

11-26

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Estados Unidos Se ha confirmado la validez de este valor de autoridad por un usuario

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Nueva York

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Fil: Del Bufalo, Donatella. Regina Elena National Cancer Institute; Italia

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Fil: Di Martile, Marta. Regina Elena National Cancer Institute; Italia

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Fil: Valentini, Elisabetta. Regina Elena National Cancer Institute; Italia

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Fil: Manni, Isabella. Regina Elena National Cancer Institute; Italia

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Fil: Masi, Ilenia. Consiglio Nazionale delle Ricerche; Italia

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Fil: D'Amore, Antonella. Università degli Studi di Roma "La Sapienza"; Italia

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Fil: Filippini, Antonio. Università degli Studi di Roma "La Sapienza"; Italia

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Fil: Nicoletti, Carmine. Università degli Studi di Roma "La Sapienza"; Italia

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Fil: Zaccarini, Marco. San Gallicano Dermatological Institute; Italia

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Fil: Cota, Carlo. San Gallicano Dermatological Institute; Italia

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Fil: Castro, María Victoria. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Maimónides. Centro de Estudios Biomédicos, Básicos, Aplicados y Desarrollo. Departamento de Ciencias Biológicas y Biomédicas; Argentina

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Fil: Quezada, Maria Josefina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Maimónides. Centro de Estudios Biomédicos, Básicos, Aplicados y Desarrollo. Departamento de Ciencias Biológicas y Biomédicas; Argentina

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Fil: Rosanò, Laura. Consiglio Nazionale delle Ricerche; Italia. Regina Elena National Cancer Institute; Italia

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Fil: Lopez Bergami, Pablo Roberto. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Maimónides. Área de Investigaciones Biomédicas y Biotecnológicas. Centro de Estudios Biomédicos, Biotecnológicos, Ambientales y de Diagnóstico; Argentina

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Fil: D'Aguanno, Simona. Regina Elena National Cancer Institute; Italia

dc.journal.title

Exploration of Targeted Anti-tumor Therapy

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info:eu-repo/semantics/altIdentifier/url/https://www.explorationpub.com/Journals/etat/Article/100268

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info:eu-repo/semantics/altIdentifier/doi/http://dx.doi.org/10.37349/etat.2022.00068

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