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Development of a personalized therapeutic strategy for ERBB-gene-mutated cancers.

Malgorzata MilewskaMattia CremonaClare MorganJohn O'SheaAoife CarrSri H VellankiAnn M HopkinsSinead ToomeyStephen F MaddenBryan T HennessyAlex J Eustace
Published in: Therapeutic advances in medical oncology (2018)
We demonstrate that ERBB family mutations are common in cancers not associated with overexpression or amplification of HER family proteins. These ERBB family mutant cancers are sensitive to treatment with PI3K inhibitors, and when combined with pan-HER inhibitors have synergistic antiproliferative effects.
Keyphrases
  • tyrosine kinase
  • copy number
  • genome wide
  • wild type
  • cancer therapy
  • young adults
  • drug delivery
  • label free
  • genome wide identification