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Pyridine-pyrimidine amides that prevent HGF-induced epithelial scattering by two distinct mechanisms |
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| Authors: | Adam Siddiqui-Jain Jacob P Hoj J Blade Hargiss Taylor H Hoj Carter J Payne Collin A Ritchie Steven R Herron Colette Quinn Jeffrey T Schuler Marc DH Hansen |
| Institution: | 1. Frost Biologic, Inc., 5201 South Green St., Suite 160, Salt Lake City, UT 84123, USA;2. Department of Physiology and Developmental Biology, Brigham Young University, 4005 LSB, Provo, UT 84602, USA;3. Structure-ase, Inc., Saratoga Springs, UT 84045, USA;4. TA Instruments, Lindon, UT 84020, USA |
| Abstract: | Stimulation of cultured epithelial cells with scatter factor/hepatocyte growth factor (HGF) results in individual cells detaching and assuming a migratory and invasive phenotype. Epithelial scattering recapitulates cancer progression and studies have implicated HGF signaling as a driver of cancer metastasis. Inhibitors of HGF signaling have been proposed to act as anti-cancer agents. We previously screened a small molecule library for compounds that block HGF-induced epithelial scattering. Most hits identified in this screen exhibit anti-mitotic properties. Here we assess the biological mechanism of a compound that blocks HGF-induced scattering with limited anti-mitotic activity. Analogs of this compound have one of two distinct activities: inhibiting either cell migration or cell proliferation with cell cycle arrest in G2/M. Each activity bears unique structure–activity relationships. The mechanism of action of anti-mitotic compounds is by inhibition of microtubule polymerization; these compounds entropically and enthalpically bind tubulin in the colchicine binding site, generating a conformational change in the tubulin dimer. |
| Keywords: | Microtubule Epithelial-mesenchymal transition (EMT) Cancer Cell migration |
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