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Interplay of opposing fate choices stalls oncogenic growth in murine skin epithelium

Madeline Sandoval, Zhe Ying, Slobodan Beronja

2021eLife11 citationsDOIOpen Access PDF

Abstract

Skin epithelium can accumulate a high burden of oncogenic mutations without morphological or functional consequences. To investigate the mechanism of oncogenic tolerance, we induced Hras G12V in single murine epidermal cells and followed them long term. We observed that Hras G12V promotes an early and transient clonal expansion driven by increased progenitor renewal that is replaced with an increase in progenitor differentiation leading to reduced growth. We attribute this dynamic effect to emergence of two populations within oncogenic clones: renewing progenitors along the edge and differentiating ones within the central core. As clone expansion is accompanied by progressive enlargement of the core and diminishment of the edge compartment, the intraclonal competition between the two populations results in stabilized oncogenic growth. To identify the molecular mechanism of Hras G12V -driven differentiation, we screened known Ras-effector in vivo and identified Rassf5 as a novel regulator of progenitor fate choice that is necessary and sufficient for oncogene-specific differentiation.

Topics & Concepts

HRASBiologyProgenitor cellCell biologyProgenitorEffectorCompartment (ship)clone (Java method)Cellular differentiationGeneticsSomatic cellCancer researchMutationStem cellGeneKRASOceanographyGeologyHippo pathway signaling and YAP/TAZCancer-related Molecular PathwaysCancer Cells and Metastasis
Interplay of opposing fate choices stalls oncogenic growth in murine skin epithelium | Litcius