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ERK3 as a BRAF-Regulated Tumor Suppressor is a New Potential Cancer Target in MelanomaChen, Minyi 05 September 2017 (has links)
No description available.
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Insights into the Role of Oncogenic BRAF in Tetraploidy and Melanoma InitiationDarp, Revati A. 09 March 2021 (has links)
Melanoma, the most lethal form of skin cancer, arises from altered cells in the melanocyte lineage, but the mechanisms by which these cells progress to melanoma are unknown. To understand the early cellular events that contribute to melanoma formation, we examined melanocytes in melanoma-prone zebrafish strains expressing BRAFV600E, the most common oncogenic form of the BRAF kinase that is mutated in nearly 50% of human melanomas. We found that, unlike wild-type melanocytes, melanocytes in transgenic BRAFV600Eanimals were binucleate and tetraploid. Furthermore, melanocytes in p53-deficient transgenic BRAFV600Eanimals exhibited 8N and greater DNA content, suggesting bypass of a p53-dependent arrest that stops cell cycle progression of tetraploid melanocytes. These data implicate tetraploids generated by increased BRAF pathway activity as contributors to melanoma initiation. Previous studies have used artificial means of generating tetraploids, raising the question of how these cells arise during actual tumor development. To gain insight into the mechanism by which BRAFV600E generates binucleate, tetraploid cells, we established an in vitro model by which such cells are generated following BRAFV600E expression. We demonstrate thatBRAFV600E-generated tetraploids arise via cytokinesis failure during mitosis due to reduced activity of the small GTPase RhoA. We also establish that oncogene-induced centrosome amplification in the G1/S phase of the cell cycle and subsequent increase in the activity of the small GTPase Rac1, partially contribute to this phenotype. These data are of significance as recent studies have shown that aneuploid progeny of tetraploid cells can be intermediates in tumor development, and deep sequencing data suggest that at least one third of melanomas and other solid tumors have undergone a whole genome doubling event during their progression. Taken together, our melanoma-prone zebrafish model and in vitro data suggest a role for BRAFV600E-inducedtetraploidy in the genesis of melanomas. To our knowledge, this is the first in vivo model showing spontaneous rise of tetraploid cells that can give rise to tumors. This novel role of the BRAF oncogene may contribute to tumorigenesis in a broader context.
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Cell type-dependent differential activation of ERK by oncogenic KRAS or BRAF in the mouse intestinal epitheliumBrandt, Raphael 10 March 2023 (has links)
Kolorektale Karzinome (CRC) zeigen eine heterogene Ätiologie. Die Progression prämaligner Vorläufer zu CRC unterscheidet (U) sich in Morphologie, molekularen Veränderungen und Interaktion mit der Tumorumgebung. CRC weisen oft onkogene Mutationen in KRAS und BRAF auf. Diese steigern die MAPK Signalwegaktivität (Mpa). Obwohl sie im selben Signalweg wirken, sind KRAS und BRAF auf die CRC-Entitäten U verteilt. Dabei ist KRAS häufiger im sogenannten konventionellen und BRAF im serratierten Weg zu CRC mutiert. In dieser Studie nutzte ich murine intestinale Organoide (iO), die induzierbare (Ind) KRAS oder BRAF Onkogene exprimieren. Große U zwischen KRAS und BRAF zeigten sich sowohl in Signaltransduktion (ST) als auch im Phänotyp. Phosphoprotein-, ERK-Reporter-, scRNA-Seq und EM-Analysen ergaben eine starke Mpa durch BRAF, die zu hoher Expression von MAPK-Zielgenen und Verlust der epithelialen Integrität führte. iO nach KRAS-Ind blieben intakt, korrelierend mit moderater, zelltypspezifischer (ZS) Mpa in sekretorischen und undifferenzierten Zellen. Die meisten Enterozyten waren Mpa-negativ. ERK-Reporter zeigten: Das ZS Muster der Mpa ist nicht nur gegenüber KRAS, sondern auch dem Entzug von Wachstumsfaktoren stabil. Dies spricht für eine intrinsische, robuste Regulierung der Mpa. BRAF-Ind Mpa setzte die ZS Regulierung der MAPK außer Kraft und schädigte das Gewebe, im Einklang mit einer oberen Grenze tolerabler Mpa. Die ZS Mpa wurde in CRC-Zelllinien bestätigt, deren Mpa durch KRAS aber nicht BRAF U ausfiel. Ferner, nutzte ich iO mit bCatenin+KRAS-Ind, um den konventionellen Weg zu CRC zu modellieren. Die Kombination führte zu synergistischen Effekten, die sich in EGFR-unabhängigem Wachstum und der
Aufhebung der ZS Mpa-Blockade äußerten, die durch eine Verschiebung der Differenzierung zu mehr Progenitorzellen bewirkt wurde. Zusammenfassend konnte ich U in der Mpa durch KRAS oder BRAF im Darmepithel feststellen, was dazu beiträgt, deren Rollen in der CRC-Genese zu bestimmen. / Colorectal cancer (CRC) is a disease with heterogeneous etiology. Premalignant lesions
follow distinct routes of progression to carcinoma reflected by differences in morphology,
molecular alterations and the tumor environment. Mutant KRAS and BRAF are frequent,
leading to MAPK pathway activation (Mpa), which is relevant for CRC therapy. Despite
acting in the same pathway, mutant KRAS and BRAF segregate to different entities, as KRAS
is more frequent in the conventional- and BRAF being specific for the serrated route to
CRC. I used murine intestinal organoids (iO) expressing inducible oncogenic KRAS or BRAF
to study the impact of oncogenes in primary cells. I found marked differences in signal
transduction and phenotype. Phospho-protein, ERK-reporter, scRNA-seq and EM data showed
strong Mpa upon BRAF induction followed by ERK-target gene expression leading to tissue
disruption. In contrast, KRAS left the tissue intact resulting in less and cell
type-dependent Mpa limited to secretory cells, a subset of late-stage enterocytes and
undifferentiated crypt cells. Most enterocytes were irresponsive to KRAS. The pattern of
Mpa was robust towards KRAS or growth factor depletion arguing in favor of intrinsic,
resilient MAPK regulation. In iO, BRAF-induced Mpa could break this cell type-specific
regulation, indicating an upper limit of tolerable Mpa. I validated these findings in CRC
cell lines that differed in Mpa in response to oncogenic KRAS but not BRAF. Finally, I
used iO expressing an inducible form of stabilized bCatenin in combination with KRAS to
mimic events frequently found in the conventional pathway to CRC. Expression of KRAS and
bCatenin synergized in driving EGFR independent growth and breaking the villus-specific
block of Mpa by altering differentiation towards progenitor cell types. In summary, this
study emphasizes differences between Mpa induced by oncogenic KRAS or BRAF which helps
clarifying their nature in different etiological routes to CRC genesis.
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