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MITF, TFEB, and TFE3 drive distinct adaptive gene expression programs and immune infiltration in melanoma

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dc.contributor.author Dias, Diogo
dc.contributor.author Oliveira, Erica
dc.contributor.author Marti-Díaz, Roman
dc.contributor.author Andrews, Sarah
dc.contributor.author Chocarro-Calvo, Ana
dc.contributor.author Bellini, Alice
dc.contributor.author Mosteo, Laura
dc.contributor.author Vivas-García, Yurena
dc.contributor.author Chauhan, Jagat
dc.contributor.author Li, Linxin
dc.contributor.author García-Martínez, José-Manuel
dc.contributor.author Rodríguez-López, José-Neptuno
dc.contributor.author Maria-Engler, Silvya-Stuchi
dc.contributor.author Kenny, Colin
dc.contributor.author Martínez-Useros, Javier
dc.contributor.author García-Jiménez, Custodia
dc.contributor.author Sánchez-del-Campo, Luis
dc.contributor.author Louphrasitthiphol, Pakavarin
dc.contributor.author Goding, Colin-R
dc.date.accessioned 2026-03-06T14:09:26Z
dc.date.available 2026-03-06T14:09:26Z
dc.date.issued 2025-12
dc.identifier.citation Dias D, Oliveira E, Martí-Díaz R, Andrews S, Chocarro-Calvo A, Bellini A, et al. MITF, TFEB, and TFE3 drive distinct adaptive gene expression programs and immune infiltration in melanoma. Cell Reports. diciembre de 2025;44(12):116499. doi:10.1016/j.celrep.2025.116499
dc.identifier.issn 2639-1856
dc.identifier.uri https://sms.carm.es/ricsmur/handle/123456789/24677
dc.description.abstract Cells can contain multiple related transcription factors targeting the same sequences, leading to potential regulatory cooperativity, redundancy, competition, or temporally regulated factor exchange. Yet, the differential biological functions of co-targeting transcription factors are poorly understood. In melanoma, three highly related transcription factors are co-expressed: the mammalian target of rapamycin complex 1 (mTORC1)-regulated TFEB and TFE3 (both key effectors of a wide range of metabolic and microenvironmental cues assumed to perform similar functions) and the microphthalmia-associated transcription factor (MITF), which controls melanoma phenotypic identity. Here, we reveal the functional specialization of MITF, TFE3, and TFEB and their impact on melanoma progression. Notably, although all bind the same sequences, each regulates different and frequently opposing gene expression programs to coordinate differentiation, metabolism, and protein synthesis and qualitatively and quantitatively impacts tumor immune infiltration. The results uncover a hierarchical cascade whereby microenvironmental stresses, including glucose limitation, lead MITF, TFEB, and TFE3 to drive distinct biologically important transcription programs that underpin phenotypic transitions in cancer.
dc.language.iso eng
dc.publisher CELL PRESS
dc.rights Atribución/Reconocimiento 4.0 Internacional
dc.rights.uri https://creativecommons.org/licenses/by/4.0/deed.es
dc.subject.mesh Microphthalmia-Associated Transcription Factor/metabolism/genetics
dc.subject.mesh Basic Helix-Loop-Helix Leucine Zipper Transcription Factors/metabolism/genetics
dc.subject.mesh Melanoma/genetics/immunology/pathology/metabolism
dc.subject.mesh Humans
dc.subject.mesh Animals
dc.subject.mesh Gene Expression Regulation, Neoplastic
dc.subject.mesh Mice
dc.subject.mesh Cell Line, Tumor
dc.title MITF, TFEB, and TFE3 drive distinct adaptive gene expression programs and immune infiltration in melanoma
dc.type info:eu-repo/semantics/article
dc.identifier.pmid 41275493
dc.relation.publisherversion https://linkinghub.elsevier.com/retrieve/pii/S2211124725012707
dc.type.version info:eu-repo/semantics/publishedVersion
dc.identifier.doi 10.1016/j.celrep.2025.116499
dc.journal.title Cell Reports
dc.identifier.essn 2211-1247


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