Your search keyword '"Sisó, Pol"' showing total 4 results

1. T-Type Calcium Channels as Potential Therapeutic Targets in Vemurafenib-Resistant BRAFV600E Melanoma

Author

Barceló, Carla, Sisó, Pol, Maiques, Oscar, García-Mulero, Sandra, Sanz-Pamplona, Rebeca, Navaridas, Raúl, Megino, Cristina, Felip, Isidre, Urdanibia, Izaskun, Eritja, Núria, Soria, Xavier, Piulats, Josep M., Penin, Rosa M., Dolcet, Xavier, Matías-Guiu, Xavier, Martí, Rosa M., and Macià, Anna

Published

2020

2. AR/D1A-deficient cells require HDAC6 for progression of endometrial carcinoma.

Author

Megino-Luque, Cristina, Sisó, Pol, Mota-Martorell, Natalia, Navaridas, Raúl, de la Rosa, Inés, Urdanibia, Izaskun, Albertí-Valls, Manel, Santacana, Maria, Pinyol, Miquel, Bonifaci, Núria, Macià, Anna, Llobet-Navas, David, Gatius, Sònia, Matias-Guiu, Xavier, and Eritja, Núria

Abstract

AT-rich interactive domain-containing protein 1A (ARID1A) loss-offunction mutation accompanied by a loss of ARID1A protein expression is frequently observed in endometrial carcinomas. However, the molecular mechanisms linking these genetic changes to the altered pathways regulating tumour initiation, maintenance and/or progression remain poorly understood. Thus, the main aim of this study was to analyse the role of ARID1A loss of function in endometrial tumorigenesis. Here, using different endometrial in vitro and in vivo models, such as tumoral cell lines, 3D primary cultures and metastatic or genetically modified mouse models, we show that altered expression of ARID1A is not enough to initiate endometrial tumorigenesis. However, in an established endometrial cancer context, ARID1A loss of function accelerates tumoral progression and metastasis through the disruption of the G2/M cell cycle checkpoint and ATM/ATRmediated DNA damage checkpoints, increases epithelial cell proliferation rates and induces epithelial mesenchymal transition through the activation of histone deacetylase 6 (HDAC6). Next, we demonstrated that the inhibition of HDAC6 function, using the HDAC6-specific inhibitor ACY1215 or by transfection with HDAC6 short hairpin RNA (shRNA), can reverse the migratory and invasive phenotype of ARIDlA-knockdown cells. Further, we also show that inhibition of HDAC6 activity causes an apoptotic vulnerability to etoposide treatments in ARIDlA-deficient cells. In summary, the findings exposed in this work indicate that the inhibition of HDAC6 activity is a potential therapeutic strategy for patients suffering from ARID1A-mutant endometrial cancer diagnosed in advanced stages. [ABSTRACT FROM AUTHOR]

Published

2022

3. BRAF V600E Mutant Allele Frequency (MAF) Influences Melanoma Clinicopathologic Characteristics.

Author

Soria, Xavier, Vilardell, Felip, Maiques, Óscar, Barceló, Carla, Sisó, Pol, de la Rosa, Inés, Velasco, Ana, Cuevas, Dolors, Santacana, Maria, Gatius, Sònia, Matías-Guiu, Xavier, Rodrigo, Alberto, Macià, Anna, and Martí, Rosa M.

Subjects

GENETIC mutation, SEQUENCE analysis, MELANOMA, ALLELES, RETROSPECTIVE studies, FISHER exact test, RESEARCH funding, PHENOTYPES

Abstract

Simple Summary: The mutational load of BRAFV600E in melanomas has been described as a possible prognostic biomarker but there is no information about the mutant allele frequency (MAF) variability of BRAFV600E within cutaneous melanomas and its potential prognostic implications. Our study suggests that the variation degree of BRAFV600E MAF within primary cutaneous melanoma could act as a determinant in the location of primary melanomas as well as their first metastases and could influence prognostic indicators such as Breslow and mitotic indexes. BRAFV600E MAF variation is also related to the neoplastic cell phenotype and tumor lymphocytic infiltrate of primary tumors. For all these reasons, detection of BRAFV600E MAF variation could be a useful prognostic biomarker. It is worth exploring the role of BRAFV600E MAF variation with regards to the response of melanoma to targeted therapies. Background: Cutaneous melanoma shows high variability regarding clinicopathological presentation, evolution and prognosis. Methods: Next generation sequencing was performed to analyze hotspot mutations in different areas of primary melanomas (MMp) and their paired metastases. Clinicopathological features were evaluated depending on the degree of variation of the BRAFV600E mutant allele frequency (MAF) in MMp. Results: In our cohort of 14 superficial spreading, 10 nodular melanomas and 52 metastases, 17/24 (71%) melanomas had a BRAFV600E mutation and 5/24 (21%) had a NRASQ61 mutation. We observed a high variation of BRAFV600E MAF (H-BRAFV600E) in 7/17 (41%) MMp. The H-BRAFV600E MMp were all located on the trunk, had lower Breslow and mitotic indexes and predominantly, a first nodal metastasis. Regions with spindled tumor cells (Spin) and high lymphocytic infiltrate (HInf) were more frequent in the H-BRAFV600E patients (4/7; 57%), whereas regions with epithelial tumor cells (Epit) and low lymphocytic infiltrate (LInf) were predominant (6/10; 60%) and exclusive in the low BRAFV600E MAF variation tumors (L-BRAFV600E). The H-BRAFV600E/Spin/HInf MMp patients had better prognostic features and nodal first metastasis. Conclusions: The H-BRAFV600E MMp were located on the trunk, had better prognostic characteristics, such as lower Breslow and mitotic indexes as well as high lymphocytic infiltrate. [ABSTRACT FROM AUTHOR]

Published

2021

4. T-Type Calcium Channels: A Potential Novel Target in Melanoma.

Author

Barceló, Carla, Sisó, Pol, Maiques, Oscar, de la Rosa, Inés, Martí, Rosa M., and Macià, Anna

Subjects

*CALCIUM, *MELANOMA, *MEMBRANE proteins, *TUMOR markers, *DISEASE progression, *CELL survival, *CELL migration inhibition

Abstract

T-type calcium channels (TTCCs) are overexpressed in several cancers. In this review, we summarize the recent advances and new insights into TTCC biology, tumor progression, and prognosis biomarker and therapeutic potential in the melanoma field. We describe a novel correlation between the Cav3.1 isoform and the increased basal autophagy in BRAFV600E-mutant melanomas and after acquired resistance to BRAF inhibitors. Indeed, TTCC blockers reduce melanoma cell viability and migration/invasion in vitro and tumor growth in mice xenografts in both BRAF-inhibitor-sensitive and -resistant scenarios. These studies open a new, promising therapeutic approach for disseminated melanoma and improved treatment in BRAFi relapsed melanomas, but further validation and clinical trials are needed for it to become a real therapeutic option. [ABSTRACT FROM AUTHOR]

Published

2020