Hijacking DNA methyltransferase transition state analogues to produce chemical scaffolds for PRMT inhibitors

被引:25
作者
Halby, Ludovic [1 ,2 ]
Marechal, Nils [3 ,4 ,5 ,6 ]
Pechalrieu, Dany [1 ]
Cura, Vincent [3 ,4 ,5 ,6 ]
Franchini, Don-Marc [1 ,16 ]
Faux, Celine [1 ]
Alby, Frederic [7 ]
Troffer-Charlier, Nathalie [3 ,4 ,5 ,6 ]
Kudithipudi, Srikanth [8 ]
Jeltsch, Albert [8 ]
Aouadi, Wahiba [9 ,10 ]
Decroly, Etienne [9 ,10 ]
Guillemot, Jean-Claude [9 ,10 ]
Page, Patrick [11 ]
Ferroud, Clotilde [12 ]
Bonnefond, Luc [3 ,4 ,5 ,6 ]
Guianvarc'h, Dominique [13 ,14 ]
Cavarelli, Jean [3 ,4 ,5 ,6 ]
Arimondo, Paola B. [1 ,15 ]
机构
[1] CNRS, ETaC FRE3600, Bat IBCG, F-31062 Toulouse, France
[2] CNRS, MEAE, Maison Francaise Oxford, 2-10 Norham Rd, Oxford, England
[3] Inst Genet & Biol Mol Cellulaire, Illkirch Graffenstaden, France
[4] CNRS, UMR7104, Illkirch Graffenstaden, France
[5] INSERM, U1258, Illkirch Graffenstaden, France
[6] Univ Strasbourg, Illkirch Graffenstaden, France
[7] Lab Pierre Fabre, 3 Ave H Curien, F-31100 Toulouse, France
[8] Univ Stuttgart, Fac Chem, Inst Biochem, Pfaffenwaldring 55, D-70569 Stuttgart, Germany
[9] Aix Marseille Univ, Lab Architecture Fonct Macromol Biol, AFMB UMR 7257, 163 Ave Luminy, F-13288 Marseille 09, France
[10] CNRS, 163 Ave Luminy, F-13288 Marseille 09, France
[11] Epiremed SAS, 1 Rue Penitents Blancs, F-31000 Toulouse, France
[12] Conservatoire Natl Arts & Metiers, EA7341, CMGPCE, Lab Chim Mol, 2 Rue Conte, F-75003 Paris, France
[13] UPMC Univ Paris 06, Sorbonne Univ, Ecole Normale Super, Lab Biomol LBM,CNRS, 4 Pl Jussieu, F-75005 Paris, France
[14] UPMC Univ Paris 06, Dept Chim, Ecole Normale Super, PSL Res Univ,Lab Biomol LBM,CNRS, F-75005 Paris, France
[15] Churchill Coll, Cambridge CB3 0DS, England
[16] Ctr Rech Cancerol Toulouse, INSERM, UMR1037, Toulouse, France
关键词
epigenetics; DNA methylation; histone methylation; transition state analogues; PRMT inhibitor; chemical probes; PROTEIN ARGININE METHYLTRANSFERASES; SMALL-MOLECULE INHIBITORS; FUNCTIONAL INSIGHTS; METHYLATION; COACTIVATOR; CARM1; EXPRESSION; TOOLS; MODEL;
D O I
10.1098/rstb.2017.0072
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
DNA, RNA and histone methylation is implicated in various human diseases such as cancer or viral infections, playing a major role in cell process regulation, especially in modulation of gene expression. Here we developed a convergent synthetic pathway starting from a protected bromomethylcytosine derivative to synthesize transition state analogues of the DNA methyltransferases. This approach led to seven 5-methylcytosine-adenosine compounds that were, surprisingly, inactive against hDNMT1, hDNMT3Acat, TRDMT1 and other RNA human and viral methyltransferases. Interestingly, compound 4 and its derivative 2 showed an inhibitory activity against PRMT4 in the micromolar range. Crystal structures showed that compound 4 binds to the PRMT4 active site, displacing strongly the S-adenosyl-L-methionine cofactor, occupying its binding site, and interacting with the arginine substrate site through the cytosine moiety that probes the space filled by a substrate peptide methylation intermediate. Furthermore, the binding of the compounds induces important structural switches, These findings open new routes for the conception of new potent PRMT4 inhibitors based on the 5-methylcytosine-adenosine scaffold. This article is part of a discussion meeting issue 'Frontiers in epigenetic chemical biology'.
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页数:15
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