Cancer Informatics (Jan 2008)

Chromosome 20q Amplification Regulates in Vitro Response to Kinesin-5 Inhibitor

  • Peter S. Linsley,
  • Steven R. Bartz,
  • Hongyue Dai,
  • Matthew Biery,
  • Teresa Ward,
  • Sumire Kobayashi,
  • Mao Mao,
  • Aimee L. Jackson

Journal volume & issue
Vol. 6
pp. 147 – 164

Abstract

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We identified gene expression signatures predicting responsiveness to a Kinesin-5 (KIF11) inhibitor (Kinesin-5i) in cultured colon tumor cell lines. Genes predicting resistance to Kinesin-5i were enriched for those from chromosome 20q, a region of frequent amplifi cation in a number of tumor types. siRNAs targeting genes in this chromosomal region identified AURKA, TPX2 and MYBL2 as genes whose disruption enhances response to Kinesin-5i. Taken together, our results show functional interaction between these genes, and suggest that their overexpression is involved in resistance to Kinesin-5i. Furthermore, our results suggest that patients whose tumors overexpress AURKA due to amplification of 20q will more likely resist treatment with Kinesin-5 inhibitor, and that inactivation of AURKA may sensitize these patients to treatment.

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