| Literature DB >> 29577543 |
Maria Castaneda1, Luxi Chen1, Lagnajeet Pradhan2, Shichang Li2, Ruba Zein1, Yeongju Lee3, Hyun-Suk Lim3, Hyun-Joo Nam2, Jiyong Lee1.
Abstract
The epithelial-mesenchymal transition (EMT) has been suggested as a new target for therapeutic intervention of metastatic cancer. Forkhead box protein C2 (FOXC2) is known to be necessary for initiating and maintaining EMT, and therefore bestows on cancer cells metastatic and cancer stem cell (CSC)-like phenotypes, allowing cells to acquire higher motility, invasiveness, self-renewal, and therapy resistance. Here, we describe the first inhibitor of FOXC2, MC-1-F2. MC-1-F2 was able to induce cadherin switching and reverse EMT through the degradation of FOXC2 and blocking of its nuclear localization. In addition, MC-1-F2 was very effective in inhibiting cancer cell migration and invasion. As the first small-molecule inhibitor of FOXC2 and the first compound targeting EMT-associated transcription factor, MC-1-F2 will pave the way for a new anticancer therapeutic agent targeting metastatic cancer and help to elucidate the network of EMT signaling pathways.Entities:
Keywords: cancer metastasis; combinatorial chemistry; drug discovery; epithelial-mesenchymal transition; transcription factor
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Year: 2018 PMID: 29577543 DOI: 10.1002/cbic.201800022
Source DB: PubMed Journal: Chembiochem ISSN: 1439-4227 Impact factor: 3.164