(R)‐PFI‐2 Analogues as Substrates and Inhibitors of Histone Lysine Methyltransferase SETD7

Author:

Porzberg Miriam R. B.12,Lenstra Danny C.2,Damen Eddy3,Blaauw Richard H.3,Rutjes Floris P. J. T.2,Wegert Anita3,Mecinović Jasmin1

Affiliation:

1. Department of Physics Chemistry and Pharmacy University of Southern Denmark Campusvej 55 5230 Odense Denmark

2. Institute for Molecules and Materials Radboud University Heyendaalseweg 135 6525 AJ Nijmegen (The Netherlands

3. Symeres Netherlands B.V. Kerkenbos 1013 6546 BB Nijmegen (The Netherlands

Abstract

Abstract(R)‐PFI‐2 is a histone substrate‐competitive inhibitor of the human histone lysine monomethyltransferase SETD7. Aimed at developing potent inhibitors of SETD7 that can also act as small molecule substrates, we replaced the pyrrolidine ring of (R)‐PFI‐2 with several side chains bearing nucleophilic functional groups. We explored the inhibitory activity of 20 novel (R)‐PFI‐2 analogues, and found that the most potent analogue has a hydroxyethyl side chain (7). SETD7’s ability to catalyse methylation of (R)‐PFI‐2‐based small molecules was evaluated by mass spectrometric assays, and we observed efficient methylation of analogues bearing lysine mimicking nucleophilic amines. The optimal side chain was found to be an aminoethyl group (1), which was surprisingly also dimethylated by SETD7. The work demonstrates that small molecules can act as both substrates and inhibitors of biomedically important SETD7.

Funder

Nederlandse Organisatie voor Wetenschappelijk Onderzoek

European Research Council

Publisher

Wiley

Subject

Organic Chemistry,General Pharmacology, Toxicology and Pharmaceutics,Molecular Medicine,Drug Discovery,Biochemistry,Pharmacology

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