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Dra. González-Pecchi, Valentina
Nombre de publicación
Dra. González-Pecchi, Valentina
Nombre completo
González Pecchi, Valentina María
Facultad
Email
vgonzalez@ucsc.cl
ORCID
9 results
Research Outputs
Now showing 1 - 9 of 9
- PublicationThe role of Epithelial-to-Mesenchymal Transition Transcription Factors (EMT-TFs) in acute myeloid Leukemia progression(MDPI, 2024); ; ; - PublicationNSD3 in cancer: Unraveling methyltransferase-dependent and isoform-specific functionsNSD3 (nuclear receptor-binding SET domain protein 3) is a member of the NSD histone methyltransferase family of proteins. In recent years, it has been identified as a potential oncogene in certain types of cancer. The NSD3 gene encodes three isoforms, the long version (NSD3L), a short version (NSD3S) and the WHISTLE isoforms. Importantly, the NSD3S isoform corresponds to the N-terminal region of the full-length protein, lacking the methyltransferase domain. The chromosomal location of NSD3 is frequently amplified across cancer types, such as breast, lung, and colon, among others. Recently, this amplification has been correlated to a chromothripsis event, that could explain the different NSD3 alterations found in cancer. The fusion proteins containing NSD3 have also been reported in leukemia (NSD3-NUP98), and in NUT (nuclear protein of the testis) midline carcinoma (NSD3-NUT). Its role as an oncogene has been described by modulating different cancer pathways through its methyltransferase activity, or the short isoform of the protein, through protein interactions. Specifically, in this review we will focus on the functions that have been characterized as methyltransferase dependent, and those that have been correlated with the expression of the NSD3S isoform. There is evidence that both the NSD3L and NSD3S isoforms are relevant for cancer progression, establishing NSD3 as a therapeutic target. However, further functional studies are needed to differentiate NSD3 oncogenic activity as dependent or independent of the catalytic domain of the protein, as well as the contribution of each isoform and its clinical significance in cancer progression.
- PublicationRole of HDAC6-STAT3 in immunomodulatory pathways in Colorectal cancer cells(Elsevier, 2023); ; ; - PublicationNSD3S stabilizes MYC through hindering its interaction with FBXW7(Chinese Academy of Sciences, 2019); - PublicationThe OncoPPi Portal: an integrative resource to explore and prioritize protein–protein interactions for cancer target discovery(2018); - PublicationDevelopment of a Time-Resolved Fluorescence Resonance Energy Transfer Ultrahigh-Throughput Screening Assay for Targeting the NSD3 and MYC Interaction(Mary Ann Liebert Inc, 2018); - PublicationOncoPPi-informed discovery of mitogen-activated protein kinase kinase 3 as a novel binding partner of c-Myc(Springer Nature, 2017); - PublicationThe OncoPPi network of cancer-focused protein–protein interactions to inform biological insights and therapeutic strategies(Springer Nature, 2017); - PublicationApolipoprotein A-I enhances proliferation of human endothelial progenitor cells and promotes angiogenesis through the cell surface ATP synthase(Springer Nature, 2015);