BMC Medical Genomics (Aug 2012)

Genetic and bioinformatic analyses of the expression and function of PI3K regulatory subunit PIK3R3 in an Asian patient gastric cancer library

  • Zhou Jin,
  • Chen Geng,
  • Tang Yew,
  • Sinha Rohit,
  • Wu Yonghui,
  • Yap Chui,
  • Wang Guihua,
  • Hu Junbo,
  • Xia Xianmin,
  • Tan Patrick,
  • Goh Liang,
  • Yen Paul

DOI
https://doi.org/10.1186/1755-8794-5-34
Journal volume & issue
Vol. 5, no. 1
p. 34

Abstract

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Abstract Background While there is strong evidence for phosphatidylinositol 3-kinase (PI3K) involvement in cancer development, there is limited information about the role of PI3K regulatory subunits. PIK3R3, the gene that encodes the PI3K regulatory subunit p55γ, is over-expressed in glioblastoma and ovarian cancers, but its expression in gastric cancer (GC) is not known. We thus used genetic and bioinformatic approaches to examine PIK3R3 expression and function in GC, the second leading cause of cancer mortality world-wide and highly prevalent among Asians. Methods Primary GC and matched non-neoplastic mucosa tissue specimens from a unique Asian patient gastric cancer library were comprehensively profiled with platforms that measured genome-wide mRNA expression, DNA copy number variation, and DNA methylation status. Function of PIK3R3 was predicted by IPA pathway analysis of co-regulated genes with PIK3R3, and further investigated by siRNA knockdown studies. Cell proliferation was estimated by crystal violet dye elution and BrdU incorporation assay. Cell cycle distribution was analysed by FACS. Results PIK3R3 was significantly up-regulated in GC specimens (n = 126, p Conclusion Using a combination of genetic, bioinformatic, and molecular biological approaches, we showed that PIK3R3 was up-regulated in GC and promoted cell cycle progression and proliferation; and thus may be a potential new therapeutic target for GC.