4.6 Article

Synthesis and greener pastures biological study of bis-thiadiazoles as potential Covid-19 drug candidates

期刊

ARABIAN JOURNAL OF CHEMISTRY
卷 15, 期 9, 页码 -

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ELSEVIER
DOI: 10.1016/j.arabjc.2022.104101

关键词

Bis-[1,2,4]thiadiazoles; Molecular docking; Binding energy; Remdesivir; Ivermectin; Drug-likeness prediction

资金

  1. KIT-Publication Fund of the Karlsruhe Institute of Technology
  2. DFG [2082/1-390761711]
  3. Science and Technology Commission of Shanghai Municipality [19440741300]

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A novel series of bis-thiadiazoles were synthesized and their binding affinity, amino acid interactions, and drug-like properties were studied in relation to COVID-19-related proteins. Some of the compounds showed comparable binding affinity and activity to the approved drugs Remdesivir and Ivermectin.
A novel series of bis-(Abdelhamid et al., 2017; Banerjee et al., 2018; Bharanidharan et al., 2022)thiadiazoles was synthesized from the reaction of precursor dimethyl 2,2'-(1,2-dipheny lethane-1,2-diylidene)-bis(hydrazine-1-carbodithioate) and hydrazonyl chlorides in ethanol under ultrasonic irradiation. Spectral tools (IR. NMR, MS, elemental analyses, molecular dynamic sim-ulation, DFT and LUMO and HOMO) were used to elucidate the structure of the isolated prod-ucts. Molecular docking for the precursor, 3 and ligands 6a-i to two COVID-19 important proteins M-pro and RdRp was compared with two approved drugs, Remdesivir and Ivermectin. The binding affinity varied between the ligands and the drugs. The highest recorded binding affinity of 6c with M-pro was (-9.2 kcal/mol), followed by 6b and 6a, (-8.9 and -8.5 kcal/mol), respectively. The lowest recorded binding affinity was (-7.0 kcal/mol) for 6 g. In comparison, the approved drugs showed binding affinity (-7.4 and -7.7 kcal/mol), for Remdesivir and Ivermectin, respectively, which are within the range of the binding affinity of our ligands. The binding affinity of the approved drug Ivermectin against RdRp recoded the highest (-8.6 kcal/mol), followed by 6a, 6 h, and 6i are the same have (-8.2 kcal/mol). The lowest reading was found for compound 3 ligand (-6.3 kcal/mol). On the other side, the amino acids also differed between the compounds studied in this project for both the viral proteins. The ligand 6a forms three H-bonds with Thr 319(A), Sr 255(A) and Arg 457(A), whereas Ivermectin forms three H-bonds with His 41(A), Gly143(A) and Gln 18(A) for viral M-pro. The RdRp amino acids residues could be divided into four groups based on the amino acids that interact with hydrogen or hydrophobic interactions. The first group contained 6d, 6b, 6 g, and Remdesivir with 1-4 hydrogen bonds and hydrophobic interactions 1 to 10. Group 2 is 6a and 6f exhibited 1 and 3 hydrogen bonds and 15 and 14 hydrophobic interactions. Group 3 has 6e and Ivermectin shows 4 and 3 hydrogen bonds, respectively and 11 hydrophobic interactions for both compounds. The last group contains ligands 3, 6c, 6 h, and 6i gave 1-3 hydro-gen bonds and 6c and 3 recorded the highest number of hydrophobic interactions, 14 for both 6c and 6 h. Pro Tox-II estimated compounds' activities as Hepatoxic, Carcinogenic and Mutagenic, revealing that 6f-h were inactive in all five similar to that found with Remdesivir and Ivermectin. The drug-likeness prediction was carried out by studying physicochemical properties, lipophilicity, size, polarity, insolubility, unsaturation, and flexibility. Generally, some properties of the ligands were comparable to that of the standards used in this study, Remdesivir and Ivermectin. (C) 2022 The Author(s). Published by Elsevier B.V. on behalf of King Saud University.

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