Scientific Reports (Jul 2018)

Hippo Signaling Pathway Dysregulation in Human Huntington’s Disease Brain and Neuronal Stem Cells

  • Kaly A. Mueller,
  • Kelly E. Glajch,
  • Megan N. Huizenga,
  • Remi A. Wilson,
  • Eric J. Granucci,
  • Amanda M. Dios,
  • Adelaide R. Tousley,
  • Maria Iuliano,
  • Elizabeth Weisman,
  • Michael J. LaQuaglia,
  • Marian DiFiglia,
  • Kimberly Kegel-Gleason,
  • Khashayar Vakili,
  • Ghazaleh Sadri-Vakili

DOI
https://doi.org/10.1038/s41598-018-29319-4
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 13

Abstract

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Abstract The Hippo signaling pathway is involved in organ size regulation and tumor suppression. Although inhibition of Hippo leads to tumorigenesis, activation of Hippo may play a role in neurodegeneration. Specifically, activation of the upstream regulator, mammalian sterile 20 (STE20)-like kinase 1 (MST1), reduces activity of the transcriptional co-activator Yes-Associated Protein (YAP), thereby mediating oxidative stress-induced neuronal death. Here, we investigated the possible role of this pathway in Huntington’s disease (HD) pathogenesis. Our results demonstrate a significant increase in phosphorylated MST1, the active form, in post-mortem HD cortex and in the brains of CAG knock-in Hdh Q111/Q111 mice. YAP nuclear localization was also decreased in HD post-mortem cortex and in neuronal stem cells derived from HD patients. Moreover, there was a significant increase in phosphorylated YAP, the inactive form, in HD post-mortem cortex and in Hdh Q111/Q111 brain. In addition, YAP was found to interact with huntingtin (Htt) and the chaperone 14-3-3, however this interaction was not altered in the presence of mutant Htt. Lastly, YAP/TEAD interactions and expression of Hippo pathway genes were altered in HD. Together, these results demonstrate that activation of MST1 together with a decrease in nuclear YAP could significantly contribute to transcriptional dysregulation in HD.