AI Article Synopsis
- Small molecules that replace ADP-ribose by binding to the Mac1 domain of the SARS-CoV-2 protein may help in developing antiviral drugs, as Mac1 aids the virus in evading detection.
- A high-throughput differential scanning fluorimetry (DSF) assay was developed to screen small libraries of drugs, revealing several promising candidates including nucleotides and steroids.
- To refine the screening process, researchers assessed melting curve shapes and fluorescence results, and they further investigated ligand binding through high-resolution structural analysis of one candidate compound.
Article Abstract
Small molecules that bind the SARS-CoV-2 nonstructural protein 3 Mac1 domain in place of ADP-ribose could be useful as molecular probes or scaffolds for COVID-19 antiviral drug discovery because Mac1 has been linked to the ability of coronaviruses to evade cellular detection. A high-throughput assay based on differential scanning fluorimetry (DSF) was therefore optimized and used to identify possible Mac1 ligands in small libraries of drugs and drug-like compounds. Numerous promising compounds included nucleotides, steroids, β-lactams, and benzimidazoles. The main drawback to this approach was that a high percentage of compounds in some libraries were found to influence the observed Mac1 melting temperature. To prioritize DSF screening hits, the shapes of the observed melting curves and initial assay fluorescence were examined, and the results were compared with virtual screens performed using AutoDock Vina. The molecular basis for alternate ligand binding was also examined by determining a structure of one of the hits, cyclic adenosine monophosphate, with atomic resolution.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7684785 | PMC |
| http://dx.doi.org/10.1177/2472555220960428 | DOI Listing |
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