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Design and Evaluation of Bispidine-Based SARS-CoV-2 Main Protease Inhibitors

Д. Н. Щербаков, Dmitry S. Baev, Mikhail A. Kalinin, Alexander I. Dalinger, V. Yu. Chirkova, S. V. Belenkaya, Aleksei Khvostov, Д.П. Крутько, Алексей В. Медведько, Ekaterina A. Volosnikova, Е. А. Шарлаева, Daniil V. Shanshin, Т. Г. Толстикова, Оlga I. Yarovaya, Rinat Maksyutov, Нариман Ф. Салахутдинов, Sergey Z. Vatsadze

2021ACS Medicinal Chemistry Letters53 citationsDOIOpen Access PDF

Abstract

For the first time, derivatives of 3,7-diazabicyclo[3.3.1]nonane (bispidine) were proposed as potential inhibitors of the SARS-CoV-2 main viral protease (3-chymotrypsin-like, 3CLpro). Based on the created pharmacophore model of the active site of the protease, a group of compounds were modeled and tested for activity against 3CLpro. The 3CLpro activity was measured using the fluorogenic substrate Dabcyl-VNSTLQSGLRK(FAM)MA; the efficiency of the proposed approach was confirmed by comparison with literature data for ebselen and disulfiram. The results of the experiments performed with bispidine compounds showed that 14 compounds exhibited activity in the concentration range 1-10 μM, and 3 samples exhibited submicromolar activity. The structure-activity relationship studies showed that the molecules containing a carbonyl group in the ninth position of the bicycle exhibited the maximum activity. Based on the experimental and theoretical results obtained, further directions for the development of this topic were proposed.

Topics & Concepts

PharmacophoreProteaseChemistrySubstrate (aquarium)StereochemistryEnzymeBiochemistryBiologyEcologyComputational Drug Discovery MethodsSynthesis and biological activityLipid Membrane Structure and Behavior
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