New benzoxazole derivatives as potential VEGFR-2 inhibitors and apoptosis inducers: design, synthesis, anti-proliferative evaluation, flowcytometric analysis, and <i>in silico</i> studies

Elkady, Hazem; Elwan, Alaa; El-Mahdy, Hesham A.; Doghish, Ahmed S.; Ismail, Ahmed; Taghour, Mohammed S; Elkaeed, Eslam B.; Eissa, Ibrahim H.; Dahab, Mohammed A.; Mahdy, Hazem A.; Khalifa, Mohamed M.

doi:10.1080/14756366.2021.2015343

Cited by 105 publications

(35 citation statements)

References 57 publications

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“…The molecular docking was conducted for compound 10 against VEGFR-2 [ 34 , 35 ] by MOE2014 software (Montreal, QC, Canada). Supplementary Materials provide a thorough explanation.…”

Section: Methodsmentioning

confidence: 99%

Design, Synthesis, Docking, DFT, MD Simulation Studies of a New Nicotinamide-Based Derivative: In Vitro Anticancer and VEGFR-2 Inhibitory Effects

et al. 2022

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A nicotinamide-based derivative was designed as an antiproliferative VEGFR-2 inhibitor with the key pharmacophoric features needed to interact with the VEGFR-2 catalytic pocket. The ability of the designed congener ((E)-N-(4-(1-(2-(4-benzamidobenzoyl)hydrazono)ethyl)phenyl)nicotinamide), compound 10, to bind with the VEGFR-2 enzyme was demonstrated by molecular docking studies. Furthermore, six various MD simulations studies established the excellent binding of compound 10 with VEGFR-2 over 100 ns, exhibiting optimum dynamics. MM-GBSA confirmed the proper binding with a total exact binding energy of −38.36 Kcal/Mol. MM-GBSA studies also revealed the crucial amino acids in the binding through the free binding energy decomposition and declared the interactions variation of compound 10 inside VEGFR-2 via the Protein–Ligand Interaction Profiler (PLIP). Being new, its molecular structure was optimized by DFT. The DFT studies also confirmed the binding mode of compound 10 with the VEGFR-2. ADMET (in silico) profiling indicated the examined compound’s acceptable range of drug-likeness. The designed compound was synthesized through the condensation of N-(4-(hydrazinecarbonyl)phenyl)benzamide with N-(4-acetylphenyl)nicotinamide, where the carbonyl group has been replaced by an imine group. The in-vitro studies were consonant with the obtained in silico results as compound 10 prohibited VEGFR-2 with an IC50 value of 51 nM. Compound 10 also showed antiproliferative effects against MCF-7 and HCT 116 cancer cell lines with IC50 values of 8.25 and 6.48 μM, revealing magnificent selectivity indexes of 12.89 and 16.41, respectively.

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“…The molecular docking was conducted for compound 10 against VEGFR-2 [ 34 , 35 ] by MOE2014 software (Montreal, QC, Canada). Supplementary Materials provide a thorough explanation.…”

Section: Methodsmentioning

confidence: 99%

Design, Synthesis, Docking, DFT, MD Simulation Studies of a New Nicotinamide-Based Derivative: In Vitro Anticancer and VEGFR-2 Inhibitory Effects

et al. 2022

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“…The assay was applied by ELISA kits in accordance with the comprehensive description in 18 , 33 as described in Supplementary data .…”

Section: Methodsmentioning

confidence: 99%

“…These previously mentioned parts enabled the designed compounds to fit perfectly in the TK active pocket. Based on the promising biological results in our former published work in which we utilised benzoxazole moieties as a hinge-binding core 18 , we decided to continue our preliminary VEGFR-2 studies using the same three different scaffolds of benzoxazole but with two main considerable additional modifications; a) For the allosteric hydrophobic pocket, we used different terminal aliphatic hydrophobic moieties including cyclopentyl (compounds 12a-c ) and ter-butyl moiety (compounds 12d-f ). This allowed us to make a comparative study between aliphatic and aromatic derivatives of each scaffold and study the SAR of the obtained compounds as anticancer leads with significant VEGFR-2 inhibitory potentialities, as was planned in our design.…”

Section: Introductionmentioning

confidence: 99%

Benzoxazole derivatives as new VEGFR-2 inhibitors and apoptosis inducers: design, synthesis, in silico studies, and antiproliferative evaluation

Taghour

Mahdy

Gomaa

et al. 2022

Journal of Enzyme Inhibition and Medicinal Chemistry

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In this study, a set of novel benzoxazole derivatives were designed, synthesised, and biologically evaluated as potential VEGFR-2 inhibitors. Five compounds ( 12d , 12f , 12i , 12l , and 13a ) displayed high growth inhibitory activities against HepG2 and MCF-7 cell lines and were further investigated for their VEGFR-2 inhibitory activities. The most potent anti-proliferative member 12 l ( IC 50 = 10.50 μM and 15.21 μM against HepG2 and MCF-7, respectively ) had the most promising VEGFR-2 inhibitory activity (IC 50 = 97.38 nM). A further biological evaluation revealed that compound 12l could arrest the HepG2 cell growth mainly at the Pre-G1 and G1 phases. Furthermore, compound 12l could induce apoptosis in HepG2 cells by 35.13%. likely, compound 12l exhibited a significant elevation in caspase-3 level (2.98-fold) and BAX (3.40-fold), and a significant reduction in Bcl-2 level (2.12-fold). Finally, docking studies indicated that 12l exhibited interactions with the key amino acids in a similar way to sorafenib.

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“…Docking studies were proceeded to inspect the binding free energies (∆G) and the binding modes [111][112][113][114][115][116] of the antiviral compounds against M pro PDB ID: 6LU7 (Table 4) with PRD_002214 as a reference. Eight compounds (128, 130, 156, 180, 184, 203, 204, and 278) exhibited the most a-like binding mode and the highest binding energies.…”

Section: Docking Studiesmentioning

confidence: 99%

Multi-Step In Silico Discovery of Natural Drugs against COVID-19 Targeting Main Protease

Youssef

Eissa

Elkady

et al. 2022

IJMS

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In continuation of our antecedent work against COVID-19, three natural compounds, namely, Luteoside C (130), Kahalalide E (184), and Streptovaricin B (278) were determined as the most promising SARS-CoV-2 main protease (Mpro) inhibitors among 310 naturally originated antiviral compounds. This was performed via a multi-step in silico method. At first, a molecular structure similarity study was done with PRD_002214, the co-crystallized ligand of Mpro (PDB ID: 6LU7), and favored thirty compounds. Subsequently, the fingerprint study performed with respect to PRD_002214 resulted in the election of sixteen compounds (7, 128, 130, 156, 157, 158, 180, 184, 203, 204, 210, 237, 264, 276, 277, and 278). Then, results of molecular docking versus Mpro PDB ID: 6LU7 favored eight compounds (128, 130, 156, 180, 184, 203, 204, and 278) based on their binding affinities. Then, in silico toxicity studies were performed for the promising compounds and revealed that all of them have good toxicity profiles. Finally, molecular dynamic (MD) simulation experiments were carried out for compounds 130, 184, and 278, which exhibited the best binding modes against Mpro. MD tests revealed that luteoside C (130) has the greatest potential to inhibit SARS-CoV-2 main protease.

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New benzoxazole derivatives as potential VEGFR-2 inhibitors and apoptosis inducers: design, synthesis, anti-proliferative evaluation, flowcytometric analysis, and in silico studies

Cited by 105 publications

References 57 publications

Design, Synthesis, Docking, DFT, MD Simulation Studies of a New Nicotinamide-Based Derivative: In Vitro Anticancer and VEGFR-2 Inhibitory Effects

Design, Synthesis, Docking, DFT, MD Simulation Studies of a New Nicotinamide-Based Derivative: In Vitro Anticancer and VEGFR-2 Inhibitory Effects

Benzoxazole derivatives as new VEGFR-2 inhibitors and apoptosis inducers: design, synthesis, in silico studies, and antiproliferative evaluation

Multi-Step In Silico Discovery of Natural Drugs against COVID-19 Targeting Main Protease

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