| Literature DB >> 28163017 |
Frank Fontaine1, Jeroen Overman1, Mehdi Moustaqil2, Sreeman Mamidyala1, Angela Salim1, Kamesh Narasimhan3, Nina Prokoph3, Avril A B Robertson1, Linda Lua4, Kirill Alexandrov1, Peter Koopman1, Robert J Capon1, Emma Sierecki2, Yann Gambin2, Ralf Jauch5, Matthew A Cooper1, Johannes Zuegg6, Mathias Francois7.
Abstract
Pharmacological modulation of transcription factors (TFs) has only met little success over the past four decades. This is mostly due to standard drug discovery approaches centered on blocking protein/DNA binding or interfering with post-translational modifications. Recent advances in the field of TF biology have revealed a central role of protein-protein interaction in their mode of action. In an attempt to modulate the activity of SOX18 TF, a known regulator of vascular growth in development and disease, we screened a marine extract library for potential small-molecule inhibitors. We identified two compounds, which inspired a series of synthetic SOX18 inhibitors, able to interfere with the SOX18 HMG DNA-binding domain, and to disrupt HMG-dependent protein-protein interaction with RBPJ. These compounds also perturbed SOX18 transcriptional activity in a cell-based reporter gene system. This approach may prove useful in developing a new class of anti-angiogenic compounds based on the inhibition of TF activity.Entities:
Keywords: SOX transcription factor; protein-DNA interaction; protein-protein interaction; salicylate; small-molecule
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Year: 2017 PMID: 28163017 DOI: 10.1016/j.chembiol.2017.01.003
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116