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Hippo pathway inactivation through subcellular localization of NF2/merlin in outer cells of mouse embryos. | LitMetric

Hippo pathway inactivation through subcellular localization of NF2/merlin in outer cells of mouse embryos.

Development

Laboratory of Animal Genetics and Reproduction, Research Faculty of Agriculture, Hokkaido University, Sapporo 060-8589, Japan.

Published: July 2024

AI Article Synopsis

  • The Hippo pathway is essential for regulating cell growth and differentiation, playing a key role in tumor development and embryonic formation.
  • Scaffold proteins from the ERM family, particularly NF2 (Merlin), influence this pathway through cell polarity, but how this works for outer cell establishment is not fully understood.
  • This study created specific Nf2 mutants to investigate its impact on YAP1 localization, revealing that NF2's positioning around the cell membrane affects cell polarity and the Hippo pathway's function by regulating the placement of proteins like LATS2 and ezrin.

Article Abstract

The Hippo pathway plays a crucial role in cell proliferation and differentiation during tumorigenesis, tissue homeostasis and early embryogenesis. Scaffold proteins from the ezrin-radixin-moesin (ERM) family, including neurofibromin 2 (NF2; Merlin), regulate the Hippo pathway through cell polarity. However, the mechanisms underlying Hippo pathway regulation via cell polarity in establishing outer cells remain unclear. In this study, we generated artificial Nf2 mutants in the N-terminal FERM domain (L64P) and examined Hippo pathway activity by assessing the subcellular localization of YAP1 in early embryos expressing these mutant mRNAs. The L64P-Nf2 mutant inhibited NF2 localization around the cell membrane, resulting in YAP1 cytoplasmic translocation in the polar cells. L64P-Nf2 expression also disrupted the apical centralization of both large tumor suppressor 2 (LATS2) and ezrin in the polar cells. Furthermore, Lats2 mutants in the FERM binding domain (L83K) inhibited YAP1 nuclear translocation. These findings demonstrate that NF2 subcellular localization mediates cell polarity establishment involving ezrin centralization. This study provides previously unreported insights into how the orchestration of the cell-surface components, including NF2, LATS2 and ezrin, modulates the Hippo pathway during cell polarization.

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Source
http://dx.doi.org/10.1242/dev.202639DOI Listing

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