LMTK3 is essential for oncogenic KIT expression in KIT-mutant GIST and melanoma
Certain cancers, including gastrointestinal stromal tumor (GIST) and subsets of melanoma, are caused by somatic KIT mutations that result in KIT receptor tyrosine kinase constitutive activity, which drives proliferation. The treatment of KIT -mutant GIST has been revolutionized with the advent of KI...
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Veröffentlicht in: | Oncogene 2019-02, Vol.38 (8), p.1200-1210 |
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Zusammenfassung: | Certain cancers, including gastrointestinal stromal tumor (GIST) and subsets of melanoma, are caused by somatic
KIT
mutations that result in KIT receptor tyrosine kinase constitutive activity, which drives proliferation. The treatment of
KIT
-mutant GIST has been revolutionized with the advent of KIT-directed cancer therapies. KIT tyrosine kinase inhibitors (TKI) are superior to conventional chemotherapy in their ability to control advanced
KIT
-mutant disease. However, these therapies have a limited duration of activity due to drug-resistant secondary
KIT
mutations that arise (or that are selected for) during KIT TKI treatment. To overcome the problem of KIT TKI resistance, we sought to identify novel therapeutic targets in
KIT
-mutant GIST and melanoma cells using a human tyrosine kinome siRNA screen. From this screen, we identified lemur tyrosine kinase 3 (
LMTK3
) and herein describe its role as a novel KIT regulator in
KIT
-mutant GIST and melanoma cells. We find that LMTK3 regulated the translation rate of KIT, such that loss of LMTK3 reduced total KIT, and thus KIT downstream signaling in cancer cells. Silencing of
LMTK3
decreased cell viability and increased cell death in KIT-dependent, but not KIT-independent GIST and melanoma cell lines. Notably,
LMTK3
silencing reduced viability of all
KIT
-mutant cell lines tested, even those with drug-resistant KIT secondary mutations. Furthermore, targeting of
LMTK3
with siRNA delayed KIT-dependent GIST growth in a xenograft model. Our data suggest the potential of LMTK3 as a target for treatment of patients with
KIT
-mutant cancer, particularly after failure of KIT TKIs. |
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ISSN: | 0950-9232 1476-5594 |
DOI: | 10.1038/s41388-018-0508-5 |