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Publication : Inactivation of the Hippo tumor suppressor pathway promotes melanoma.

First Author  Vittoria MA Year  2022
Journal  Nat Commun Volume  13
Issue  1 Pages  3732
PubMed ID  35768444 Mgi Jnum  J:326521
Mgi Id  MGI:7313481 Doi  10.1038/s41467-022-31399-w
Citation  Vittoria MA, et al. (2022) Inactivation of the Hippo tumor suppressor pathway promotes melanoma. Nat Commun 13(1):3732
abstractText  Melanoma is commonly driven by activating mutations in the MAP kinase BRAF; however, oncogenic BRAF alone is insufficient to promote melanomagenesis. Instead, its expression induces a transient proliferative burst that ultimately ceases with the development of benign nevi comprised of growth-arrested melanocytes. The tumor suppressive mechanisms that restrain nevus melanocyte proliferation remain poorly understood. Here we utilize cell and murine models to demonstrate that oncogenic BRAF leads to activation of the Hippo tumor suppressor pathway, both in melanocytes in vitro and nevus melanocytes in vivo. Mechanistically, we show that oncogenic BRAF promotes both ERK-dependent alterations in the actin cytoskeleton and whole-genome doubling events, which independently reduce RhoA activity to promote Hippo activation. We also demonstrate that functional impairment of the Hippo pathway enables oncogenic BRAF-expressing melanocytes to bypass nevus formation and rapidly form melanomas. Our data reveal that the Hippo pathway enforces the stable arrest of nevus melanocytes and represents a critical barrier to melanoma development.
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