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KRC-327, a selective novel inhibitor of c-Met receptor tyrosine kinase with anticancer activity

Authors :
Jae Wook Ryu
Kyung Hee Jung
Soon-Sun Hong
Byung Hee Park
Sun-Mi Yun
Sang-Won Hong
Jongkook Lee
Hee Jung Jung
Jae Du Ha
Source :
Cancer Letters. 331:158-166
Publication Year :
2013
Publisher :
Elsevier BV, 2013.

Abstract

c-Met receptor tyrosine kinase and its ligand, hepatocyte growth factor (HGF), have been reported to be involved in tumorigenesis and metastatic progression. We synthesized a novel triazolopyridazine derivative KRC-327 which selectively targets the c-Met. When we performed receptor tyrosine kinases (RTKs) array with 42 different phosphorylated-RTKs, KRC-327 strongly inhibited expression of activated c-Met in MKN-45 cancer cells. This was confirmed by immunofluorescence staining. Also, KRC-327 decreased the expression of Gab1, Akt, signal transducer and activator of transcription 3 (STAT3) and Erk, down-stream signals of c-Met. KRC-327 strongly suppressed the growth of c-Met over-expressed cancer cells (MKN-45, SNU-638, SNU-5), while not in c-Met absent cancer cell lines (MKN-1, SNU-1). Furthermore, KRC-327 effectively induced cell cycle arrest, especially G0/G1 arrest by increasing expression of p21, p27 and decreasing that of cyclin D1. In the ligand-induced functional studies, KRC-327 inhibited proliferation of HGF-stimulated BxPC-3 cells, the migration of HGF-stimulated AGS cancer cells, and suppressed colony formation in HGF-stimulated U-87MG cells. In xenograft animal models, KRC-327 significantly not only delayed tumor growth but also suppressed phosphorylation of c-Met and its signaling cascades as well as proliferation. Taken together, these results demonstrate that KRC-327 selectively targets c-Met, resulting in inhibition of cell growth and proliferation. Therefore, we suggest that KRC-327 may be a novel drug candidate with the therapeutic potential of targeting c-Met in human cancer.

Details

ISSN :
03043835
Volume :
331
Database :
OpenAIRE
Journal :
Cancer Letters
Accession number :
edsair.doi.dedup.....2926bd9f7c9dd618c43ae2e31bacde5e