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  3. Differential inhibition sensitivities of MET mutants to the small molecule inhibitor SU11274
 

Differential inhibition sensitivities of MET mutants to the small molecule inhibitor SU11274

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Publisher DOI
10.1016/j.canlet.2009.08.017
PubMed ID
19783361
Description
Point mutations emerge as one of the rate-limiting steps in tumor response to small molecule inhibitors of protein kinases. Here we characterized the response of the MET mutated variants, V1110I, V1238I, V1206L and H1112L to the small molecule SU11274. Our results reveal a distinct inhibition pattern of the four mutations with IC(50) values for autophosphorylation inhibition ranging between 0.15 and 1.5muM. Differences were further seen on the ability of SU11274 to inhibit phosphorylation of downstream MET transducers such as AKT, ERK, PLCgamma and STAT3 and a variety of MET-dependent biological endpoints. In all the assays, H1112L was the most sensitive to SU11274, while V1206L was less affected under the used concentration range. The differences in responses to SU11274 are discussed based on a structural model of the MET kinase domain.
Date of Publication
2010
Publication Type
Article
Language(s)
en
Contributor(s)
Zimmer, Yitzhak
Universitätsklinik für Radio-Onkologie
Vaseva, Angelina V
Medova, Michaela
Universitätsklinik für Radio-Onkologie
Streit, Bruno
Blank-Liss, Wieslawa
Greiner, Richard H
Schiering, Nikolaus
Aebersold, Daniel Matthiasorcid-logo
Universitätsklinik für Radio-Onkologie
Additional Credits
Universitätsklinik für Radio-Onkologie
Series
Cancer letters
Publisher
Elsevier
ISSN
0304-3835
Access(Rights)
metadata.only
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