PLoS ONE (Jan 2014)

p120RasGAP is a mediator of rho pathway activation and tumorigenicity in the DLD1 colorectal cancer cell line.

  • Shawna L Organ,
  • Josephine Hai,
  • Nikolina Radulovich,
  • Christopher B Marshall,
  • Lisa Leung,
  • Takehiko Sasazuki,
  • Senji Shirasawa,
  • Chang-Qi Zhu,
  • Roya Navab,
  • Mitsuhiko Ikura,
  • Ming-Sound Tsao

DOI
https://doi.org/10.1371/journal.pone.0086103
Journal volume & issue
Vol. 9, no. 1
p. e86103

Abstract

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KRAS is mutated in ∼40% of colorectal cancer (CRC), and there are limited effective treatments for advanced KRAS mutant CRC. Therefore, it is crucial that downstream mediators of oncogenic KRAS continue to be studied. We identified p190RhoGAP as being phosphorylated in the DLD1 CRC cell line, which expresses a heterozygous KRAS G13D allele, and not in DKO4 in which the mutant allele has been deleted by somatic recombination. We found that a ubiquitous binding partner of p190RhoGAP, p120RasGAP (RasGAP), is expressed in much lower levels in DKO4 cells compared to DLD1, and this expression is regulated by KRAS. Rescue of RasGAP expression in DKO4 rescued Rho pathway activation and partially rescued tumorigenicity in DKO4 cells, indicating that the combination of mutant KRAS and RasGAP expression is crucial to these phenotypes. We conclude that RasGAP is an important effector of mutant KRAS in CRC.