PLoS ONE (Jan 2011)

Neuropilin-2 mediated β-catenin signaling and survival in human gastro-intestinal cancer cell lines.

  • Shaija Samuel,
  • Puja Gaur,
  • Fan Fan,
  • Ling Xia,
  • Michael J Gray,
  • Nikolaos A Dallas,
  • Debashish Bose,
  • Cristian Rodriguez-Aguayo,
  • Gabriel Lopez-Berestein,
  • Greg Plowman,
  • Anil Bagri,
  • Anil K Sood,
  • Lee M Ellis

DOI
https://doi.org/10.1371/journal.pone.0023208
Journal volume & issue
Vol. 6, no. 10
p. e23208

Abstract

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NRP-2 is a high-affinity kinase-deficient receptor for ligands belonging to the class 3 semaphorin and vascular endothelial growth factor families. NRP-2 has been detected on the surface of several types of human cancer cells, but its expression and function in gastrointestinal (GI) cancer cells remains to be determined. We sought to determine the function of NRP-2 in mediating downstream signals regulating the growth and survival of human gastrointestinal cancer cells. In human gastric cancer specimens, NRP-2 expression was detected in tumor tissues but not in adjacent normal mucosa. In CNDT 2.5 cells, shRNA mediated knockdown NRP-2 expression led to decreased migration and invasion in vitro (p<0.01). Focused gene-array analysis demonstrated that loss of NRP-2 reduced the expression of a critical metastasis mediator gene, S100A4. Steady-state levels and function of β-catenin, a known regulator of S100A4, were also decreased in the shNRP-2 clones. Furthermore, knockdown of NRP-2 sensitized CNDT 2.5 cells in vitro to 5FU toxicity. This effect was associated with activation of caspases 3 and 7, cleavage of PARP, and downregulation of Bcl-2. In vivo growth of CNDT 2.5 cells in the livers of nude mice was significantly decreased in the shNRP-2 group (p<0.05). Intraperitoneal administration of NRP-2 siRNA-DOPC decreased the tumor burden in mice (p = 0.01). Collectively, our results demonstrate that tumor cell-derived NRP-2 mediates critical survival signaling in gastrointestinal cancer cells.