A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors

Lei L. Chen; Jonathan C. Trent; Elsie F. Wu; Gregory N. Fuller; Latha Ramdas; Wei Zhang; Austin K. Raymond; Victor G. Prieto; Caroline O. Oyedeji; Kelly K. Hunt; Raphael E. Pollock; Barry W. Feig; Kimberly J. Hayes; Haesun Choi; Homer A. Macapinlac; Walter Hittelman; Marco A. Velasco; Shreyaskumar Patel; Michael A. Burgess; Robert S. Benjamin; Marsha L. Frazier

doi:10.1158/0008-5472.CAN-04-0085

A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors

Lei L. Chen, Jonathan C. Trent, Elsie F. Wu, Gregory N. Fuller, Latha Ramdas, Wei Zhang, Austin K. Raymond, Victor G. Prieto, Caroline O. Oyedeji, Kelly K. Hunt, Raphael E. Pollock, Barry W. Feig, Kimberly J. Hayes, Haesun Choi, Homer A. Macapinlac, Walter Hittelman, Marco A. Velasco, Shreyaskumar Patel, Michael A. Burgess, Robert S. BenjaminMarsha L. Frazier

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313 Scopus citations

Abstract

KIT gain of function mutations play an important role in the pathogenesis of gastrointestinal stromal tumors (GISTs). Imatinib is a selective tyrosine kinase inhibitor of ABL, platelet-derived growth factor receptor (PDGFR), and KIT and represents a new paradigm of targeted therapy against GISTs. Here we report for the first time that, after imatinib treatment, an additional specific and novel KIT mutation occurs in GISTs as they develop resistance to the drug. We studied 12 GIST patients with initial near-complete response to imatinib. Seven harbored mutations in KIT exon 11, and 5 harbored mutations in exon 9. Within 31 months, six imatinib-resistant rapidly progressive peritoneal implants (metastatic foci) developed in five patients. Quiescent residual GISTs persisted in seven patients. All six rapidly progressive imatinib-resistant implants from five patients show an identical novel KIT missense mutation, 1982T→C, that resulted in Val654Ala in KIT tyrosine kinase domain 1. This novel mutation has never been reported before, is not present in pre-imatinib or post-imatinib residual quiescent GISTs, and is strongly correlated with imatinib resistance. Allelic-specific sequencing data show that this new mutation occurs in the allele that harbors original activation mutation of KIT.

Original language	English (US)
Pages (from-to)	5913-5919
Number of pages	7
Journal	Cancer Research
Volume	64
Issue number	17
DOIs	https://doi.org/10.1158/0008-5472.CAN-04-0085
State	Published - Sep 1 2004

ASJC Scopus subject areas

Oncology
Cancer Research

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Chen, L. L., Trent, J. C., Wu, E. F., Fuller, G. N., Ramdas, L., Zhang, W., Raymond, A. K., Prieto, V. G., Oyedeji, C. O., Hunt, K. K., Pollock, R. E., Feig, B. W., Hayes, K. J., Choi, H., Macapinlac, H. A., Hittelman, W., Velasco, M. A., Patel, S., Burgess, M. A., ... Frazier, M. L. (2004). A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors. Cancer Research, 64(17), 5913-5919. https://doi.org/10.1158/0008-5472.CAN-04-0085

Chen, LL, Trent, JC, Wu, EF, Fuller, GN, Ramdas, L, Zhang, W, Raymond, AK, Prieto, VG, Oyedeji, CO, Hunt, KK, Pollock, RE, Feig, BW, Hayes, KJ, Choi, H , Macapinlac, HA, Hittelman, W, Velasco, MA, Patel, S, Burgess, MA, Benjamin, RS & Frazier, ML 2004, 'A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors', Cancer Research, vol. 64, no. 17, pp. 5913-5919. https://doi.org/10.1158/0008-5472.CAN-04-0085

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title = "A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors",

abstract = "KIT gain of function mutations play an important role in the pathogenesis of gastrointestinal stromal tumors (GISTs). Imatinib is a selective tyrosine kinase inhibitor of ABL, platelet-derived growth factor receptor (PDGFR), and KIT and represents a new paradigm of targeted therapy against GISTs. Here we report for the first time that, after imatinib treatment, an additional specific and novel KIT mutation occurs in GISTs as they develop resistance to the drug. We studied 12 GIST patients with initial near-complete response to imatinib. Seven harbored mutations in KIT exon 11, and 5 harbored mutations in exon 9. Within 31 months, six imatinib-resistant rapidly progressive peritoneal implants (metastatic foci) developed in five patients. Quiescent residual GISTs persisted in seven patients. All six rapidly progressive imatinib-resistant implants from five patients show an identical novel KIT missense mutation, 1982T→C, that resulted in Val654Ala in KIT tyrosine kinase domain 1. This novel mutation has never been reported before, is not present in pre-imatinib or post-imatinib residual quiescent GISTs, and is strongly correlated with imatinib resistance. Allelic-specific sequencing data show that this new mutation occurs in the allele that harbors original activation mutation of KIT.",

author = "Chen, {Lei L.} and Trent, {Jonathan C.} and Wu, {Elsie F.} and Fuller, {Gregory N.} and Latha Ramdas and Wei Zhang and Raymond, {Austin K.} and Prieto, {Victor G.} and Oyedeji, {Caroline O.} and Hunt, {Kelly K.} and Pollock, {Raphael E.} and Feig, {Barry W.} and Hayes, {Kimberly J.} and Haesun Choi and Macapinlac, {Homer A.} and Walter Hittelman and Velasco, {Marco A.} and Shreyaskumar Patel and Burgess, {Michael A.} and Benjamin, {Robert S.} and Frazier, {Marsha L.}",

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AU - Chen, Lei L.

AU - Trent, Jonathan C.

AU - Wu, Elsie F.

AU - Fuller, Gregory N.

AU - Ramdas, Latha

AU - Zhang, Wei

AU - Raymond, Austin K.

AU - Prieto, Victor G.

AU - Oyedeji, Caroline O.

AU - Hunt, Kelly K.

AU - Pollock, Raphael E.

AU - Feig, Barry W.

AU - Hayes, Kimberly J.

AU - Choi, Haesun

AU - Macapinlac, Homer A.

AU - Hittelman, Walter

AU - Velasco, Marco A.

AU - Patel, Shreyaskumar

AU - Burgess, Michael A.

AU - Benjamin, Robert S.

AU - Frazier, Marsha L.

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N2 - KIT gain of function mutations play an important role in the pathogenesis of gastrointestinal stromal tumors (GISTs). Imatinib is a selective tyrosine kinase inhibitor of ABL, platelet-derived growth factor receptor (PDGFR), and KIT and represents a new paradigm of targeted therapy against GISTs. Here we report for the first time that, after imatinib treatment, an additional specific and novel KIT mutation occurs in GISTs as they develop resistance to the drug. We studied 12 GIST patients with initial near-complete response to imatinib. Seven harbored mutations in KIT exon 11, and 5 harbored mutations in exon 9. Within 31 months, six imatinib-resistant rapidly progressive peritoneal implants (metastatic foci) developed in five patients. Quiescent residual GISTs persisted in seven patients. All six rapidly progressive imatinib-resistant implants from five patients show an identical novel KIT missense mutation, 1982T→C, that resulted in Val654Ala in KIT tyrosine kinase domain 1. This novel mutation has never been reported before, is not present in pre-imatinib or post-imatinib residual quiescent GISTs, and is strongly correlated with imatinib resistance. Allelic-specific sequencing data show that this new mutation occurs in the allele that harbors original activation mutation of KIT.

AB - KIT gain of function mutations play an important role in the pathogenesis of gastrointestinal stromal tumors (GISTs). Imatinib is a selective tyrosine kinase inhibitor of ABL, platelet-derived growth factor receptor (PDGFR), and KIT and represents a new paradigm of targeted therapy against GISTs. Here we report for the first time that, after imatinib treatment, an additional specific and novel KIT mutation occurs in GISTs as they develop resistance to the drug. We studied 12 GIST patients with initial near-complete response to imatinib. Seven harbored mutations in KIT exon 11, and 5 harbored mutations in exon 9. Within 31 months, six imatinib-resistant rapidly progressive peritoneal implants (metastatic foci) developed in five patients. Quiescent residual GISTs persisted in seven patients. All six rapidly progressive imatinib-resistant implants from five patients show an identical novel KIT missense mutation, 1982T→C, that resulted in Val654Ala in KIT tyrosine kinase domain 1. This novel mutation has never been reported before, is not present in pre-imatinib or post-imatinib residual quiescent GISTs, and is strongly correlated with imatinib resistance. Allelic-specific sequencing data show that this new mutation occurs in the allele that harbors original activation mutation of KIT.

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ER -

A missense mutation in KIT kinase domain 1 correlates with imatinib resistance in gastrointestinal stromal tumors

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