Cancers (Nov 2020)

Targeting the RhoGEF βPIX/COOL-1 in Glioblastoma: Proof of Concept Studies

  • Kate Connor,
  • David W. Murray,
  • Monika A. Jarzabek,
  • Nhan L. Tran,
  • Kieron White,
  • Patrick Dicker,
  • Kieron J. Sweeney,
  • Philip J. O’Halloran,
  • Brian MacCarthy,
  • Liam P. Shiels,
  • Francesca Lodi,
  • Diether Lambrechts,
  • Jann N. Sarkaria,
  • Raymond M. Schiffelers,
  • Marc Symons,
  • Annette T. Byrne

DOI
https://doi.org/10.3390/cancers12123531
Journal volume & issue
Vol. 12, no. 12
p. 3531

Abstract

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Glioblastoma (GBM), a highly invasive and vascular malignancy is shown to rapidly develop resistance and evolve to a more invasive phenotype following bevacizumab (Bev) therapy. Rho Guanine Nucleotide Exchange Factor proteins (RhoGEFs) are mediators of key components in Bev resistance pathways, GBM and Bev-induced invasion. To identify GEFs with enhanced mRNA expression in the leading edge of GBM tumours, a cohort of GEFs was assessed using a clinical dataset. The GEF βPix/COOL-1 was identified, and the functional effect of gene depletion assessed using 3D-boyden chamber, proliferation, and colony formation assays in GBM cells. Anti-angiogenic effects were assessed in endothelial cells using tube formation and wound healing assays. In vivo effects of βPix/COOL-1-siRNA delivered via RGD-Nanoparticle in combination with Bev was studied in an invasive model of GBM. We found that siRNA-mediated knockdown of βPix/COOL-1 in vitro decreased cell invasion, proliferation and increased apoptosis in GBM cell lines. Moreover βPix/COOL-1 mediated endothelial cell migration in vitro. Mice treated with βPix/COOL-1 siRNA-loaded RGD-Nanoparticle and Bev demonstrated a trend towards improved median survival compared with Bev monotherapy. Our hypothesis generating study suggests that the RhoGEF βPix/COOL-1 may represent a target of vulnerability in GBM, in particular to improve Bev efficacy.

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