Design and synthesis of unprecedented 9- and 10-membered cyclonucleosides with PRMT5 inhibitory activity

Bioorg Med Chem. 2022 Jul 15;66:116820. doi: 10.1016/j.bmc.2022.116820.

Shuhei Kawamura ¹, Rachel L Palte ², Hai-Young Kim ³, Josep Saurí ³, Christopher Sondey ⁴, My S Mansueto ⁴, Michael D Altman ², Michelle R Machacek ⁵

Affiliations

1 Discovery Chemistry, Merck & Co., Inc., Boston, MA 02115, United States. Electronic address: [email protected].
2 Computational and Structural Chemistry, Merck & Co., Inc., Boston, MA 02115, United States.
3 NMR Structure Elucidation, Process and Analytical Chemistry, Merck & Co., Inc., Boston, MA 02115, United States.
4 Quantitative Biosciences, Merck & Co., Inc., Boston, MA 02115, United States.
5 Discovery Chemistry, Merck & Co., Inc., Boston, MA 02115, United States.

PMID: 35594650 DOI: 10.1016/j.bmc.2022.116820

Abstract

Synthesis of medium-sized rings is known to be challenging due to high transannular strain especially for 9- and 10-membered rings. Herein we report design and synthesis of unprecedented 9- and 10-membered purine 8,5'-cyclonucleosides as the first cyclonucleoside PRMT5 inhibitors. The cocrystal structure of PRMT5:MEP50 in complex with the synthesized 9-membered cyclonucleoside 1 revealed its binding mode in the SAM binding pocket of PRMT5.

Keywords

Cyclonucleoside; Medicinal chemistry; Molecular modeling; Nucleoside; PRMT5; PRMT5 inhibitor; X-ray crystallography.

Products

Cat. No.

Product Name

Description

Target

Research Area
HY-150081

PRMT5-IN-21

PRMT5 Inhibitor

Histone Methyltransferase

Cancer

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