Novel adamantyl clubbed iminothiazolidinones as promising elastase inhibitors: design, synthesis, molecular docking, ADMET and DFT studies

Ahmed, Atteeque; Saeed, Aamer; Ejaz, Syeda Abida; Aziz, Mubashir; Hashmi, Muhammad Zaffar; Channar, Pervaiz Ali; Abbas, Qamar; Raza, Hussain; Shafiq, Zahid; El‐Seedi, Hesham R.

doi:10.1039/d1ra09318e

Cited by 31 publications

(15 citation statements)

References 42 publications

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“…The six lead molecules which have passed the Lipinski rule of five ( Table 14 ) were further assessed with other drug-likeness filter rules such as the Ghose filter rule, Veber’s rule, Egan’s rule, and Muegge’s rule using the SwissADME web server as shown in Table 15 . Lipinski's criteria for drug-likeness include molecular weight (MW ≤ 500 g/mol), n-octanol/water distribution coefficient (Log P ≤ 5), number of hydrogen bond acceptors (nHA ≤10), and number of hydrogen bond donors (nHD ≤5) ( Ahmed et al., 2022 ; Chauhan et al., 2014 ). From Lipinski's table of the lead molecules in the data set, the Log P scores of the molecules are relatively close to 3 log mol/L (optimal limit) except for molecule 17 which is slightly above the optimal limit (0 < Log P < 3).…”

Section: Resultsmentioning

confidence: 99%

“…Some of the relevant computed ADMET parameters include human intestinal absorption (HIA), human colon adenocarcinoma cell lines (Caco-2) permeability, Madin−Darby Canine Kidney cells (MDCK) permeability, plasma glycoprotein (Pgp) inhibitor, plasma glycoprotein (Pgp) substrate, plasma protein binding (PPB), volume distribution (VD), blood-brain barrier (BBB) penetration, human cytochromes (CYP), clearance (CL), half-life (T1/2), AMES toxicity, carcinogenicity (Carc), eye irritation (EI), respiratory toxicity (RT) as shown in Table 16 . The Caco-2 cell permeability has been an important index for an eligible drug candidate which is associated with human intestinal absorption ( Ahmed et al., 2022 ). The lead compounds were considered to have proper Caco-2 cell permeability because their values are higher than the optimal score of 5.15 log cm/s.…”

Section: Resultsmentioning

confidence: 99%

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RETRACTED: In-silico modelling studies of 5-benzyl-4-thiazolinone derivatives as influenza neuraminidase inhibitors via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

Abdullahi

Uzairu

Shallangwa

et al. 2022

Heliyon

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

RETRACTED: In-silico modelling studies of 5-benzyl-4-thiazolinone derivatives as influenza neuraminidase inhibitors via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

Abdullahi

Uzairu

Shallangwa

et al. 2022

Heliyon

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“…The synthesis of imino-thiazolidinone derivatives were carried out according to a Scheme 1 [ 25 ] synthetic approach. Using DCM as a solvent, substituted benzoic acids were transformed to matching acid chlorides.…”

Section: Resultsmentioning

confidence: 99%

Design, Synthesis, Kinetic Analysis and Pharmacophore-Directed Discovery of 3-Ethylaniline Hybrid Imino-Thiazolidinone as Potential Inhibitor of Carbonic Anhydrase II: An Emerging Biological Target for Treatment of Cancer

et al. 2022

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Carbonic anhydrases (CA), having Zn2+ metal atoms, are responsible for the catalysis of CO2 and water to bicarbonate and protons. Any abnormality in the functioning of these enzymes may lead to morbidities such as glaucoma and different types of cancers including brain, renal and pancreatic carcinomas. To cope with the lack of presence of a promising therapeutic agent against these cancers, searching for an efficient and suitable carbonic anhydrase inhibitor is crucial. In the current study, ten novel 3-ethylaniline hybrid imino-thiazolidinones were synthesized and characterized by FTIR, NMR (1H, 13C), and mass spectrometry. Synthesis was carried out by diethyl but-2-ynedioate cyclization and different acyl thiourea substitutions of 3-ethyl amine. The CA (II) enzyme inhibition profile for all synthesized derivatives was determined. It was observed that compound 6e demonstrated highest inhibition of CA-II with an IC50 value of 1.545 ± 0.016 µM. In order to explore the pharmacophoric properties and develop structure activity relationship, in silico screening was performed. In silico investigations included density functional theory (DFT) studies, pharmacophore-guided model development, molecular docking, molecular dynamic (MD) simulations, and prediction of drug likeness scores. DFT investigations provided insight into the electronic characteristics of compounds, while molecular docking determined the binding orientation of derivatives within the CA-II active site. Compounds 6a, 6e, and 6g had a reactive profile and generated stable protein-ligand interactions with respective docking scores of −6.12, −6.99, and −6.76 kcal/mol. MD simulations were used to evaluate the stability of the top-ranked complex. In addition, pharmacophore-guided modeling demonstrated that compound 6e produced the best pharmacophore model (HHAAARR) compared to standard brinzolamide. In vitro and in silico investigations anticipated that compound 6e would be an inhibitor of carbonic anhydrase II with high efficacy. Compound 6e may serve as a potential lead for future synthesis that can be investigated at the molecular level, and additional in vivo studies are strongly encouraged.

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“…The computed value for HIA showed that the lead compounds have the probability of excellent absorption from the intestinal membrane. The Caco-2 cell permeability has been an important index for an eligible drug candidate which is associated with human intestinal absorption [46]. The lead compounds were considered to have proper Caco-2 cell permeability because their values are higher than the optimal score of − 5.15 log cm/s.…”

Section: Drug-likeness Assessment and Admet Predictionsmentioning

confidence: 99%

“…rule, Egan'rule, and Muegge's rule using the SwissADME Web server as shown in Table15. Lipinski's criteria for drug-likeness include molecular weight (MW ≤ 500 g/ mol), n-octanol/water distribution coefficient (Log P ≤ 5), number of hydrogen bond acceptors (nHA ≤ 10), and number of hydrogen bond donors (nHD ≤ 5)[45,46].…”

mentioning

confidence: 99%

Computational modelling studies of some 1,3-thiazine derivatives as anti-influenza inhibitors targeting H1N1 neuraminidase via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

Abdullahi

Uzairu

Shallangwa

et al. 2022

Beni-Suef Univ J Basic Appl Sci

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Background Influenza virus disease remains one of the most contagious diseases that aided the deaths of many patients, especially in this COVID-19 pandemic era. Recent discoveries have shown that the high prevalence of influenza and SARS-CoV-2 coinfection can rapidly increase the death rate of patients. Hence, it became necessary to search for more potent inhibitors for influenza disease therapy. The present study utilized some computational modeling concepts such as 2D-QSAR, 3D-QSAR, molecular docking simulation, and ADMET predictions of some 1,3-thiazine derivatives as inhibitors of influenza neuraminidase (NA). Results The 2D-QSAR modeling results showed GFA-MLR ($$R_{{\text{train }}}^{2}$$ R train 2 = 0.9192, Q2 = 0.8767, R2adj = 0.8991, RMSE = 0.0959, $$R_{{{\text{test}}}}^{2}$$ R test 2 = 0.8943, $$R_{{{\text{pred}}}}^{2}$$ R pred 2 = 0.7745) and GFA-ANN ($$R_{{\text{train }}}^{2}$$ R train 2 = 0.9227, Q2 = 0.9212, RMSE = 0.0940, $$R_{{{\text{test}}}}^{2}$$ R test 2 = 0.8831, $$R_{{{\text{pred}}}}^{2}$$ R pred 2 = 0.7763) models with the computed descriptors as ATS7s, SpMax5_Bhv, nHBint6, and TDB9m for predicting the NA inhibitory activities of compounds which have passed the global criteria of accepting QSAR model. The 3D-QSAR modeling was carried out based on the comparative molecular field analysis (CoMFA) and comparative similarity indices analysis (CoMSIA). The CoMFA_ES ($$R_{{\text{train }}}^{2}$$ R train 2 = 0.9620, Q2 = 0.643) and CoMSIA_SED ($$R_{{\text{train }}}^{2}$$ R train 2 = 0.8770, Q2 = 0.702) models were found to also have good and reliable predicting ability. The compounds were also virtually screened based on their binding scores via molecular docking simulations with the active site of the NA (H1N1) target receptor which also confirms their resilient potency. Four potential lead compounds (4, 7, 14, and 15) with the relatively high inhibitory rate (> 50%) and docking (> − 6.3 kcal/mol) scores were identified as the possible lead candidates for in silico exploration of improved anti-influenza agents. Conclusion The drug-likeness and ADMET predictions of the lead compounds revealed non-violation of Lipinski’s rule and good pharmacokinetic profiles as important guidelines for rational drug design. Hence, the outcome of this research set a course for the in silico design and exploration of novel NA inhibitors with improved potency.

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Novel adamantyl clubbed iminothiazolidinones as promising elastase inhibitors: design, synthesis, molecular docking, ADMET and DFT studies

Abstract: Structurally diverse adamantyl-iminothiazolidinone conjugates were synthesized, evaluated for elastase inhibition, and subjected to in silico ADMET prediction. The inhibition studies revealed compounds 5a, 5f, 5g, and 5h to show significant activity.

Cited by 31 publications

References 42 publications

RETRACTED: In-silico modelling studies of 5-benzyl-4-thiazolinone derivatives as influenza neuraminidase inhibitors via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

RETRACTED: In-silico modelling studies of 5-benzyl-4-thiazolinone derivatives as influenza neuraminidase inhibitors via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

Design, Synthesis, Kinetic Analysis and Pharmacophore-Directed Discovery of 3-Ethylaniline Hybrid Imino-Thiazolidinone as Potential Inhibitor of Carbonic Anhydrase II: An Emerging Biological Target for Treatment of Cancer

Computational modelling studies of some 1,3-thiazine derivatives as anti-influenza inhibitors targeting H1N1 neuraminidase via 2D-QSAR, 3D-QSAR, molecular docking, and ADMET predictions

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