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Author
Niechi, Ignacio; Erices, José I.; Carrillo-Beltrán, Diego; Uribe-Ojeda, Atenea; Torres, Ángelo; Rocha, José Dellis; Uribe, Daniel; Toro, María A.; Villalobos-Nova, Karla; Gaete-Ramírez, Belén; Mingo, Gabriel; Owen, Gareth I.; Varas-Godoy, Manuel; Jara, Lilian; Aguayo, Francisco; Burzio, Verónica A.; Quezada-Monrás, Claudia; Tapia, Julio C. |
ISSN:
2073-4409 |
Language:
eng |
Date:
2023-02 |
Type:
Artículo |
Revista:
Cells |
Datos de la publicación:
vol. 12 Issue: no. 3 Pages: |
DOI:
10.3390/cells12030506 |
Description:
Publisher Copyright: © 2023 by the authors. |
Abstract:
Glioblastoma (GBM) is the most common and aggressive type of brain tumor due to its elevated recurrence following treatments. This is mainly mediated by a subpopulation of cells with stemness traits termed glioblastoma stem-like cells (GSCs), which are extremely resistant to anti-neoplastic drugs. Thus, an advancement in the understanding of the molecular processes underlying GSC occurrence should contribute significantly towards progress in reducing aggressiveness. High levels of endothelin-converting enzyme-1 (ECE1), key for endothelin-1 (ET-1) peptide activation, have been linked to the malignant progression of GBM. There are four known isoforms of ECE1 that activate ET-1, which only differ in their cytoplasmic N-terminal sequences. Isoform ECE1c is phosphorylated at Ser-18 and Ser-20 by protein kinase CK2, which increases its stability and hence promotes aggressiveness traits in colon cancer cells. In order to study whether ECE1c exerts a malignant effect in GBM, we designed an ECE1c mutant by switching a putative ubiquitination lysine proximal to the phospho-serines Lys-6-to-Arg (i.e., K6R). This ECE1cK6R mutant was stably expressed in U87MG, T98G, and U251 GBM cells, and their behavior was compared to either mock or wild-type ECE1c-expressing clone cells. ECE1cK6R behaved as a highly stable protein in all cell lines, and its expression promoted self-renewal and the enrichment of a stem-like population characterized by enhanced neurospheroid formation, as well as increased expression of stem-like surface markers. These ECE1cK6R-derived GSC-like cells also displayed enhanced resistance to the GBM-related chemotherapy drugs temozolomide and gemcitabine and increased expression of the ABCG2 efflux pump. In addition, ECE1cK6R cells displayed enhanced metastasis-associated traits, such as the modulation of adhesion and the enhancement of cell migration and invasion. In conclusion, the acquisition of a GSC-like phenotype, together with heightened chemoresistance and invasiveness traits, allows us to suggest phospho-ECE1c as a novel marker for poor prognosis as well as a potential therapeutic target for GBM. |
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