Development of a yeast-based system to identify new hBRAFV600E functional interactors

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Author(s): Tiziana Cervelli; Elena Tantillo; J. Silvio Gutkind; Laura Comelli; Federica Gemignani; Simone Lubrano; Laura Poliseno; Chiara Piccirilli; Mario Chiariello; Giorgio Cozza; Giovanna Chiorino; Francesca Dapporto; Andrea Marranci; Alvaro Galli; Alessandra Salvetti
Source:
Oncogene. 38:1355-1366
Subject Terms:
Proto-Oncogene Proteins B-raf; 0301 basic medicine; Cancer Research; Saccharomyces cerevisiae Proteins; MAP Kinase Signaling System; Saccharomyces cerevisiae; Mutant; medicine.disease_cause; Cell Line; Mitochondrial Proteins; 03 medical and health sciences; 0302 clinical medicine; Cell Line, Tumor; Genetics; medicine; Animals; Humans; Vemurafenib; Protein kinase A; Melanoma; Protein Kinase Inhibitors; Molecular Biology; Gene Library; Mutation; Tumor; biology; MAP kinase kinase kinase; Kinase; Membrane Proteins; biology.organism_classification; Yeast; Cell biology; 030104 developmental biology; 030220 oncology & carcinogenesis; Mitogen-Activated Protein Kinases; medicine.drug
Online Access:
https://explore.openaire.eu/search/publication?articleId=doi_dedup___::84c1e14b5f9a86bea130e9d6334481e4
https://doi.org/10.1038/s41388-018-0496-5

Additional Information
- Publication Information:
  Springer Science and Business Media LLC, 2018.
- Publication Date:
  2018
- Abstract:
  BRAFV600E is a mutant Ser-Thr protein kinase that plays a crucial role in many types of cancer, including melanoma. Despite several aspects of BRAFV600E biology have been already elucidated, the proteins that regulate its expression and activity remain largely unknown, hampering our capacity to control its unrestrained effects. Here, we propose yeast Saccharomyces cerevisiae as a model system that can be used to achieve a better understanding of the regulation of human BRAFV600E.By showing that in osmotic stress conditions hBRAFV600E can rescue the growth of strains carrying a double or triple deletion in MAPKKK belonging to the HOG pathway, we demonstrate that this oncogenic kinase is active in yeast even if it does not have an ortholog. Moreover, we report that, in the yeast ptp3∆ptc1∆ strain that is deleted in the genes encoding for two phosphatases responsible for Hog1 de-phoshorylation, hBRAFV600E mimics the toxicity observed in the presence of constitutive Hog1 activation. Finally, we exploit such a toxicity to perform a functional screening of a human cDNA library, looking for cDNAs able to rescue yeast growth. In this way, we identify SMIM10, a mitochondrial protein that in melanoma cells selectively downregulates BRAFV600E RNA and protein levels, by acting indirectly at the post-transcriptional level. Upon SMIM10 overexpression, BRAFV600E melanoma cells show disrupted mitochondrial structure/function and undergo senescence. They also show decreased ability to proliferate and form colonies, as well as increased sensitivity to the BRAF inhibitor vemurafenib. Interestingly, the analysis of TCGA melanoma samples indicates that patients with higher SMIM10 levels have a better prognosis. Therefore, these data suggest that SMIM10 exerts an oncosuppressive role in melanoma cells.Taken together, our results unveil the potential of S. cerevisiae to study hBRAFV600E, to populate the network of its functional interactors and, in doing so, to uncover new cancer-associated genes with therapeutic potential.
- ISSN:
  1476-5594
  0950-9232
- Rights:
  CLOSED
- Accession Number:
  edsair.doi.dedup.....84c1e14b5f9a86bea130e9d6334481e4

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