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Antiviral drug discovery with an optimized biochemical dengue protease assay: Improved predictive power for antiviral efficacy.

作者信息

Lang Johannes, Dutta Sudip Kumar, Leuthold Mila M, Reichert Lisa, Kühl Nikos, Martina Byron, Klein Christian D

机构信息

Medicinal Chemistry, Institute of Pharmacy and Molecular Biotechnology IPMB, Heidelberg University, Im Neuenheimer Feld 364, D-69120, Heidelberg, Germany.

Artemis Bioservices, Molengraaffsingel 10, 2629 JD, Delft, the Netherlands.

出版信息

Antiviral Res. 2025 Feb;234:106053. doi: 10.1016/j.antiviral.2024.106053. Epub 2024 Dec 5.

DOI:10.1016/j.antiviral.2024.106053
PMID:39645089
Abstract

The viral NS2B-NS3 protease is a promising drug target to combat dengue virus (DENV) and other emerging flaviviruses. The discovery of novel DENV protease inhibitors with antiviral efficacy is hampered by the low predictive power of biochemical assays. We herein present a comparative evaluation of biochemical DENV protease assay conditions and their benchmarking against antiviral efficacy and a protease-specific reporter gene assay. Variations were performed with respect to pH, type of detergent, buffer, and substrate. The revised assay conditions were applied in a medicinal chemistry effort aimed at phenylglycine protease inhibitors. This validation study demonstrated a considerably improved predictive power for antiviral efficacy in comparison to previous approaches. An extensive evaluation of phenylglycine-based DENV protease inhibitors with highly diverse N-terminal caps indicates further development potential in this structural region. Furthermore, the phenylglycine moiety may be less essential than previously assumed, providing a development option towards reduced lipophilicity and thereby an improved pharmacokinetic and toxicity profile.

摘要

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