Optimization of N-Piperidinyl-Benzimidazolone Derivatives as Potent and Selective Inhibitors of 8-Oxo-Guanine DNA Glycosylase 1

Olov Wallner; Armando Cázares-Körner; Emma Rose Scaletti; Geoffrey Masuyer; Tove Bekkhus; Torkild Visnes; Kirill Mamonov; Florian Ortis; Thomas Lundbäck; Maria Volkova; Tobias Koolmeister; Elisée Wiita; Olga Loseva; Monica Pandey; Evert Homan; Carlos Benítez-Buelga; Jonathan Davies; Martin Scobie; Ulrika Warpman Berglund; Christina Kalderén; Pål Stenmark; Thomas Helleday; Maurice Michel

doi:10.1002/cmdc.202200310

Optimization of N-Piperidinyl-Benzimidazolone Derivatives as Potent and Selective Inhibitors of 8-Oxo-Guanine DNA Glycosylase 1

ChemMedChem. 2023 Jan 3;18(1):e202200310. doi: 10.1002/cmdc.202200310. Epub 2022 Oct 13.

Authors

Olov Wallner¹, Armando Cázares-Körner¹, Emma Rose Scaletti², Geoffrey Masuyer², Tove Bekkhus¹, Torkild Visnes^{1

3}, Kirill Mamonov¹, Florian Ortis¹, Thomas Lundbäck⁴, Maria Volkova¹, Tobias Koolmeister¹, Elisée Wiita¹, Olga Loseva¹, Monica Pandey¹, Evert Homan¹, Carlos Benítez-Buelga^{1

5}, Jonathan Davies², Martin Scobie^{1

6}, Ulrika Warpman Berglund^{1

6}, Christina Kalderén^{1

6}, Pål Stenmark^{2

7}, Thomas Helleday^{1

8}, Maurice Michel¹

Affiliations

¹ Science for Life Laboratory, Department of Oncology-Pathology, Karolinska Institutet, 171 77, Stockholm, Sweden.
² Department of Biochemistry and Biophysics, Stockholm University, 10691, Stockholm, Sweden.
³ Department of Biotechnology and Nanomedicine, SINTEF Industry, 7465, Trondheim, Norway.
⁴ Chemical Biology Consortium Sweden (CBCS), Science for Life Laboratory, Department of Medical Biochemistry and Biophysics, Karolinska Institutet, 171 77, Stockholm, Sweden.
⁵ Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), Madrid, Spain.
⁶ Oxcia AB, 113 34, Stockholm, Sweden.
⁷ Department of Experimental Medical Science, Lund University, 221 00, Lund, Sweden.
⁸ Sheffield Cancer Centre, Department of Oncology and Metabolism, University of Sheffield, S10 2TN, Sheffield, UK.

Abstract

8-oxo Guanine DNA Glycosylase 1 is the initiating enzyme within base excision repair and removes oxidized guanines from damaged DNA. Since unrepaired 8-oxoG could lead to G : C→T : A transversion, base removal is of utmost importance for cells to ensure genomic integrity. For cells with elevated levels of reactive oxygen species this dependency is further increased. In the past we and others have validated OGG1 as a target for inhibitors to treat cancer and inflammation. Here, we present the optimization campaign that led to the broadly used tool compound TH5487. Based on results from a small molecule screening campaign, we performed hit to lead expansion and arrived at potent and selective substituted N-piperidinyl-benzimidazolones. Using X-ray crystallography data, we describe the surprising binding mode of the most potent member of the class, TH8535. Here, the N-Piperidinyl-linker adopts a chair instead of a boat conformation which was found for weaker analogues. We further demonstrate cellular target engagement and efficacy of TH8535 against a number of cancer cell lines.

Keywords: 8-oxo guanine DNA glycoslyase 1; Base excision repair; Inhibitors; OGG1; TH5487.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Benzimidazoles / pharmacology
DNA Damage
DNA Glycosylases* / chemistry
DNA Glycosylases* / genetics
DNA Glycosylases* / metabolism
DNA Repair
Guanine / chemistry
Guanine / metabolism
Humans
Neoplasms*

Substances

DNA Glycosylases
Guanine
benzimidazolone
Benzimidazoles