| Literature DB >> 31212132 |
Stephanie M Myers1, Duncan C Miller1, Lauren Molyneux1, Mercedes Arasta2, Ruth H Bawn1, Timothy J Blackburn1, Simon J Cook3, Noel Edwards2, Jane A Endicott2, Bernard T Golding1, Roger J Griffin1, Tim Hammonds4, Ian R Hardcastle1, Suzannah J Harnor1, Amy B Heptinstall1, Pamela A Lochhead3, Mathew P Martin2, Nick C Martin1, David R Newell2, Paul J Owen4, Leon C Pang4, Tristan Reuillon1, Laurent J M Rigoreau5, Huw D Thomas2, Julie A Tucker2, Lan-Zhen Wang2, Ai-Ching Wong4, Martin E M Noble6, Stephen R Wedge7, Celine Cano8.
Abstract
Extracellular regulated kinase 5 (ERK5) signalling has been implicated in driving a number of cellular phenotypes including endothelial cell angiogenesis and tumour cell motility. Novel ERK5 inhibitors were identified using high throughput screening, with a series of pyrrole-2-carboxamides substituted at the 4-position with an aroyl group being found to exhibit IC50 values in the micromolar range, but having no selectivity against p38α MAP kinase. Truncation of the N-substituent marginally enhanced potency (∼3-fold) against ERK5, but importantly attenuated inhibition of p38α. Systematic variation of the substituents on the aroyl group led to the selective inhibitor 4-(2-bromo-6-fluorobenzoyl)-N-(pyridin-3-yl)-1H-pyrrole-2-carboxamide (IC50 0.82 μM for ERK5; IC50 > 120 μM for p38α). The crystal structure (PDB 5O7I) of this compound in complex with ERK5 has been solved. This compound was orally bioavailable and inhibited bFGF-driven Matrigel plug angiogenesis and tumour xenograft growth. The selective ERK5 inhibitor described herein provides a lead for further development into a tool compound for more extensive studies seeking to examine the role of ERK5 signalling in cancer and other diseases.Entities:
Keywords: BMK1; Bioavailable; ERK5; Extracellular regulated kinase 5; Kinase; Pyrrole carboxamide
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Year: 2019 PMID: 31212132 DOI: 10.1016/j.ejmech.2019.05.057
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514