High throughput chemical screening reveals multiple regulatory proteins on FOXA1 in breast cancer cell lines

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Cited 6 times in Scopus logo

Cited 6 times in Web of Science logo

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This research was funded by NFR-young talenged grant number [250554/F20].

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Hurtado Rodríguez, AntoniAutor (correspondencia)

8 de octubre de 2019

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Artículo

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Publicado en:International Journal Of Molecular Sciences. 19 (12): - 2018-01-01 19(12), DOI: 10.3390/ijms19124123.

Autores: Wang S, Singh SK, Katika MR, Lopez-Aviles S, Hurtado A

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Resumen

Forkhead box A1 (FOXA1) belongs to the forkhead class transcription factor family, playing pioneering function for hormone receptors in breast and prostate cancers, and mediating activation of linage specific enhancers. Interplay between FOXA1 and breast cancer specific signaling pathways has been reported previously, indicating a regulation network on FOXA1 in breast cancer cells. Here in this study, we aimed to identify which are the proteins that could potentially control FOXA1 function in breast cancer cell lines expressing different molecular markers. We first established a luciferase reporter system reflecting FOXA1 binding to DNA. Then, we applied high throughput chemical screening of multiple protein targets and mass spectrometry in breast cancer cell lines expressing different molecular markers: ER positive/HER2 negative (MCF-7), ER positive/HER2 positive (BT474), and ER negative/HER2 positive (MDA-MB-453). Regardless of estrogen receptor status, HER2 (human epidermal growth factor receptor 2) enriched cell lines showed similar response to kinase inhibitors, indicating the control of FOXA1 by cell signaling kinases. Among these kinases, we identified additional receptor tyrosine kinases and cyclin-dependent kinases as regulators of FOXA1. Furthermore, we performed proteomics experiments from FOXA1 inmunoprecipitated protein complex to identify that FOXA1 interacts with several proteins. Among all the targets, we identified cyclin-dependent kinase 1 (CDK1) as a positive factor to interact with FOXA1 in BT474 cell line. In silico analyses confirmed that cyclin-dependent kinases might be the kinases responsible for FOXA1 phosphorylation at the Forkhead domain and the transactivation domain. These results reveal that FOXA1 is potentially regulated by multiple kinases. The cell cycle control kinase CDK1 might control directly FOXA1 by phosphorylation and other kinases indirectly by means of regulating other proteins.

Palabras clave

breast cancerfoxa1Breast cancerDeterminantDrug screening and proteomicsEndocrine resistanceEstrogen-receptor bindingExpressionFoxa1Hnf3Transcription factors

Indicios de calidad

Impacto bibliométrico. Análisis de la aportación y canal de difusión

El trabajo ha sido publicado en la revista International Journal Of Molecular Sciences debido a la progresión y el buen impacto que ha alcanzado en los últimos años, según la agencia Scopus (SJR), se ha convertido en una referencia en su campo. En el año de publicación del trabajo, 2018, se encontraba en la posición , consiguiendo con ello situarse como revista Q1 (Primer Cuartil), en la categoría Computer Science Applications. Destacable, igualmente, el hecho de que la Revista está posicionada por encima del Percentil 90.

2025-08-02:

WoS: 6
Scopus: 6

Impacto y visibilidad social

Análisis de liderazgo de los autores institucionales

Este trabajo se ha realizado con colaboración internacional, concretamente con investigadores de: Norway.

Existe un liderazgo significativo ya que algunos de los autores pertenecientes a la institución aparecen como primer o último firmante, se puede apreciar en el detalle: Último Autor (Hurtado Rodríguez, Antoni).