EXEL-7647 Inhibits Mutant Forms of ErbB2 Associated with Lapatinib Resistance and Neoplastic Transformation

DOI PDF 被引用文献6件
  • Torsten Trowe
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Sotiria Boukouvala
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Keith Calkins
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Richard E. Cutler
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Ryan Fong
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Roel Funke
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Steven B. Gendreau
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Yong D. Kim
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Nicole Miller
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • John R. Woolfrey
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Valentina Vysotskaia
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Jing Ping Yang
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Mary E. Gerritsen
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • David J. Matthews
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Peter Lamb
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California
  • Timothy S. Heuer
    Authors' Affiliation: Exelixis, Inc., South San Francisco, California

書誌事項

公開日
2008-04-15
DOI
  • 10.1158/1078-0432.ccr-07-4367
公開者
American Association for Cancer Research (AACR)

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説明

<jats:title>Abstract</jats:title> <jats:p>Purpose: Mutations associated with resistance to kinase inhibition are an important mechanism of intrinsic or acquired loss of clinical efficacy for kinase-targeted therapeutics. We report the prospective discovery of ErbB2 mutations that confer resistance to the small-molecule inhibitor lapatinib.</jats:p> <jats:p>Experimental Design: We did in vitro screening using a randomly mutagenized ErbB2 expression library in Ba/F3 cells, which were dependent on ErbB2 activity for survival and growth.</jats:p> <jats:p>Results: Lapatinib resistance screens identified mutations at 16 different ErbB2 amino acid residues, with 12 mutated amino acids mapping to the kinase domain. Mutations conferring the greatest lapatinib resistance cluster in the NH2-terminal kinase lobe and hinge region. Structural computer modeling studies suggest that lapatinib resistance is caused by multiple mechanisms; including direct steric interference and restriction of conformational flexibility (the inactive state required for lapatinib binding is energetically unfavorable). ErbB2 T798I imparts the strongest lapatinib resistance effect and is analogous to the epidermal growth factor receptor T790M, ABL T315I, and cKIT T670I gatekeeper mutations that are associated with clinical drug resistance. ErbB2 mutants associated with lapatinib resistance transformed NIH-3T3 cells, including L755S and T733I mutations known to occur in human breast and gastric carcinomas, supporting a direct mechanism for lapatinib resistance in ErbB2-driven human cancers. The epidermal growth factor receptor/ErbB2/vascular endothelial growth factor receptor inhibitor EXEL-7647 was found to inhibit almost all lapatinib resistance-associated mutations. Furthermore, no ErbB2 mutations were found to be associated with EXEL-7647 resistance and lapatinib sensitivity.</jats:p> <jats:p>Conclusions: Taken together, these data suggest potential target-based mechanisms of resistance to lapatinib and suggest that EXEL-7647 may be able to circumvent these effects.</jats:p>

収録刊行物

  • Clinical Cancer Research

    Clinical Cancer Research 14 (8), 2465-2475, 2008-04-15

    American Association for Cancer Research (AACR)

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