Peptidomimetic Phenoxymethyl Ketone Warheads as Potent Dual-Mode Inhibitors against SARS-CoV-2 M pro and Cathepsin.

Publication date

2025-06-12

Authors

Porzberg, Miriam R B
Groenewold, G J Mirjam
Lyoo, HeyrhyoungISNI 0000000492805278
Jakob, Alexander K M H
Titulaer, Willem H C
Cavina, Lorenzo
Poelaert, Katrien C KISNI 0000000512567124
Zwaagstra, MarleenISNI 0000000493076986
Dieteren, Cindy E J
Lemmers, Jaap G H

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Advisors

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Document Type

Article
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License

cc_by

Abstract

Five years after the onset of the COVID-19 pandemic, there still is an unmet need for novel antivirals to battle SARS-CoV-2 and other coronaviruses. For this purpose, the development of peptidomimetics against the SARS-CoV-2 main protease (M pro) and host proteases human cathepsin L (hCTSL) and cathepsin B (hCTSB) is an attractive strategy. These dual-mode antivirals target both viral entry and replication, which could be a suitable alternative to highly specific M pro and CTS inhibitors. Herein, we examined the inhibitory activity, physicochemical and ADME properties, metabolic stability, and in vivo PK parameters of peptidomimetic inhibitors bearing a potent phenoxymethyl ketone warhead. Our compounds showed nanomolar inhibition of both M pro and hCTSL/hCTSB and efficiently inhibited SARS-CoV-2 replication in cell culture. Furthermore, we studied metabolism and the impact of coadministration with the CYP-inhibitor ritonavir. Taken together, we report 1 as broad-spectrum coronavirus inhibitor with attractive properties to be pursued in in vivo efficacy studies.

Keywords

Molecular Medicine, Drug Discovery

Citation

Porzberg, M R B, Groenewold, G J M, Lyoo, H, Jakob, A K M H, Titulaer, W H C, Cavina, L, Poelaert, K C K, Zwaagstra, M, Dieteren, C E J, Lemmers, J G H, Hamdani, S H, van Buuren, B N M, Ackerschott, B, Platteeuw, J, Michorius, J, Martina, B E E, Feiters, M C, Gironés, D, van Kuppeveld, F J M, van Hemert, M J & Rutjes, F P J T 2025, 'Peptidomimetic Phenoxymethyl Ketone Warheads as Potent Dual-Mode Inhibitors against SARS-CoV-2 M pro and Cathepsin.', Journal of Medicinal Chemistry, vol. 68, no. 11, pp. 10953-10969. https://doi.org/10.1021/acs.jmedchem.4c03147