Abstract

The Michael addition reaction is a spontaneous and quick chemical reaction that is widely applied in various fields. This reaction is performed by conjugating an addition of nucleophiles with α, β-unsaturated carbonyl compounds, resulting in the bond formation of C-N, C-S, C-O, and so on. In the development of molecular materials, the Michael addition is not only used to synthesize chemical compounds but is also involved in the mechanism of drug action. Several covalent drugs that bond via Michael addition are regarded as anticarcinogens and anti-inflammatory drugs. Although drug development is mainly focused on pharmaceutical drug discovery, target-based discovery can provide a different perspective for drug usage. However, considerable time and labor are required to define a molecular target through molecular biological experiments. In this review, we systematically examine the chemical structures of current FDA-approved antiviral drugs for potential Michael addition moieties with α, β-unsaturated carbonyl groups, which may exert an unidentified broad-spectrum inhibitory mechanism to target viral or host factors. We thus propose that profiling the targets of antiviral agents, such as Michael addition products, can be achieved by employing a high-throughput LC-MS approach to comprehensively analyze the interaction between drugs and targets, and the subsequent drug responses in the cellular environment to facilitate drug repurposing and/or identify potential adverse effects, with a particular emphasis on the pros and cons of this shotgun proteomic approach.

Highlights

  • Some antiviral drugs find it difficult to undergo Michael addition owing to the inappropriate regiostructure or electron transition, the others have a high probability of acting as spontaneous Michael acceptors

  • We propose that the identification of these potential interactions in combination with the application of existing principles of medicinal chemistry and high-throughput proteomics opens a new avenue for antiviral drug development

  • Identification of a molecular target requires a longer period to explore the mechanism of drug action in pathogens and/or hosts [82]; clarification of the detailed capabilities of drugs is beneficial to enhance the feasibility of drug usage and to develop drugs to fight against subsequent resistant viruses

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Summary

Michael Addition

The various pairs of acceptors and nucleophiles of Michael addition provide diverse prospects in the development of organic synthesis and materials science, it results in many challenges in clinical medicine, especially in drug discovery because of high costs incurred, owing to the labor required and the complicated experiments that are performed. Some antiviral drugs find it difficult to undergo Michael addition owing to the inappropriate regiostructure or electron transition, the others have a high probability of acting as spontaneous Michael acceptors These compounds may have additional modes of action in addition to known functions via lower specific covalent bonding in various viral infections.

Retroviral Integrase Inhibitors
Influenza Neuraminidase Inhibitors
Enterovirus 3C Protease Inhibitors
Non-Nucleoside Reverse-Transcriptase Inhibitors and Nucleoside Analogs
C-C Chemokine Receptor Type 5 Inhibitors
Discovery of Michael Addition Drugs by Using High-Throughput
Discussion
Conclusions
Methods

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