Your search keyword '"El-Miligy MMM"' showing total 9 results

1. Discovery of new thymol-3,4-disubstituted thiazole hybrids as dual COX-2/5-LOX inhibitors with in vivo proof.

Author

El-Miligy MMM, Al-Kubeisi AK, Nassra RA, El-Zemity SR, and Hazzaa AA

Subjects

Rats, Animals, Cyclooxygenase 2 metabolism, Celecoxib, Thiazoles pharmacology, Cyclooxygenase 1 metabolism, Molecular Docking Simulation, Lipoxygenase Inhibitors pharmacology, Structure-Activity Relationship, Molecular Structure, Cyclooxygenase 2 Inhibitors pharmacology, Thymol pharmacology

Abstract

New thymol-3,4-disubstitutedthiazole hybrids were synthesised as dual COX-2/5-LOX inhibitors. Compounds 6b , 6d , 6e , and 6f displayed in vitro inhibitory activity against COX-2 (IC 50 = 0.037, 0.042, 0.046, and 0.039 µM ) nearly equal to celecoxib (IC 50 = 0.045 µM ) . 6b , 6d , and 6f showed SI (379, 341, and 374, respectively) higher than that of celecoxib (327). 6a - l elicited in vitro 5-LOX inhibitory activity higher than quercetin. 6a - f , 6i - l , 7a , and 7c possessed in vivo inhibition of formalin induced paw edoema higher than celecoxib. 6a , 6b , 6f , 6h - l , and 7b showed gastrointestinal safety profile as celecoxib and diclofenac sodium in the population of fasted rats. Induced fit docking and molecular dynamics simulation predicted good fitting of 6b and 6f without changing the packing and globularity of the apo protein. In conclusion, 6b and 6f achieved the target goal as multitarget inhibitors of inflammation.

Published

2024

2. Imparting aromaticity to 2-pyridone derivatives by O -alkylation resulted in new competitive and non-competitive PIM-1 kinase inhibitors with caspase-activated apoptosis.

Author

Abdelaziz ME, El-Miligy MMM, Fahmy SM, Abu-Serie MM, Hazzaa AA, and Mahran MA

Subjects

Humans, Proto-Oncogene Proteins c-pim-1 chemistry, Proto-Oncogene Proteins c-pim-1 metabolism, Caspases metabolism, Cell Line, Tumor, Protein Kinase Inhibitors chemistry, Caco-2 Cells, Kinetics, Ligands, Apoptosis, Cell Proliferation, Molecular Docking Simulation, Drug Screening Assays, Antitumor, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Antineoplastic Agents chemistry, Pyridones

Abstract

New aromatic O -alkyl pyridine derivatives were designed and synthesised as Proviral Integration Moloney (PIM)-1 kinase inhibitors. 4c and 4f showed potent in vitro anticancer activity against NFS-60, HepG-2, PC-3, and Caco-2 cell lines and low toxicity against normal human lung fibroblast Wi-38 cell line. Moreover, 4c and 4f induced apoptosis in the four tested cancer cell lines with high percentage. In addition, 4c and 4f significantly induced caspase 3/7 activation in HepG-2 cell line. Furthermore, 4c and 4f showed potent PIM-1 kinase inhibitory activity with IC 50  = 0.110, 0.095 µM, respectively. Kinetic studies indicated that 4c and 4f were both competitive and non-competitive inhibitors for PIM-1 kinase enzyme. In addition, in silico prediction of physiochemical properties, pharmacokinetic profile, ligand efficiency, ligand lipophilic efficiency, and induced fit docking studies were consistent with the biological and kinetic studies, and predicted that 4c and 4f could act as PIM-1 kinase competitive non-adenosine triphosphate (ATP) mimetics with drug like properties.

Published

2024

3. Discovery of new pyridine-quinoline hybrids as competitive and non-competitive PIM-1 kinase inhibitors with apoptosis induction and caspase 3/7 activation capabilities.

Author

El-Miligy MMM, Abdelaziz ME, Fahmy SM, Ibrahim TM, Abu-Serie MM, Mahran MA, and Hazzaa AA

Subjects

Male, Humans, Proto-Oncogene Proteins c-pim-1 metabolism, Proto-Oncogene Proteins c-pim-1 pharmacology, Caspase 3 metabolism, Molecular Docking Simulation, Cell Line, Tumor, Kinetics, Caco-2 Cells, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors metabolism, Pyridines pharmacology, Apoptosis, Cell Proliferation, Drug Screening Assays, Antitumor, Antineoplastic Agents pharmacology, Quinolines pharmacology

Abstract

New quinoline-pyridine hybrids were designed and synthesised as PIM-1/2 kinase inhibitors. Compounds 5b , 5c , 6e, 13a , 13c, and 14a showed in-vitro low cytotoxicity against normal human lung fibroblast Wi-38 cell line and potent in-vitro anticancer activity against myeloid leukaemia (NFS-60), liver (HepG-2), prostate (PC-3), and colon (Caco-2) cancer cell lines. In addition, 6e, 13a, and 13c significantly induced apoptosis with percentage more than 66%. Moreover, 6e, 13a, and 13c significantly induced caspase 3/7 activation in HepG-2 cell line. Furthermore, 5c, 6e, and 14a showed potent in-vitro PIM-1 kinase inhibitory activity. While, 5b showed potent in-vitro PIM-2 kinase inhibitory activity. Kinetic studies using Lineweaver-Burk double-reciprocal plot indicated that 5b , 5c , 6e, and 14a behaved as competitive inhibitors while 13a behaved as both competitive and non-competitive inhibitor of PIM-1 kinase enzyme. Molecular docking studies indicated that, in-silico affinity came in coherence with the observed in-vitro inhibitory activities against PIM-1/2 kinases.

Published

2023

4. Towards safer anti-inflammatory therapy: synthesis of new thymol-pyrazole hybrids as dual COX-2/5-LOX inhibitors.

Author

El-Miligy MMM, Al-Kubeisi AK, Bekhit MG, El-Zemity SR, Nassra RA, and Hazzaa AA

Subjects

Rats, Animals, Cyclooxygenase 2, Lipoxygenase Inhibitors pharmacology, Celecoxib pharmacology, Quercetin, Molecular Docking Simulation, Anti-Inflammatory Agents pharmacology, Pyrazoles pharmacology, Cyclooxygenase 2 Inhibitors pharmacology, Thymol

Abstract

New thymol - 1,5-disubstitutedpyrazole hybrids were synthesised as dual COX-2/5-LOX inhibitors. Compounds 8b , 8g , 8c, and 4a displayed in vitro inhibitory activity against COX-2 (IC 50  = 0.043, 0.045, 0.063, and 0.068 µM ) nearly equal to celecoxib (IC 50  = 0.045 µM ) with high SI (316, 268, 204, and 151, respectively) comparable to celecoxib (327). All target compounds, 4a-c and 8a-i , showed in vitro 5-LOX inhibitory activity higher than reference quercetin. Besides, they possessed in vivo inhibition of formalin-induced paw oedema higher than celecoxib. In addition, compounds 4a, 4b, 8b, and 8g showed superior gastrointestinal safety profile (no ulceration) as celecoxib and diclofenac sodium in the population of fasted rats. In conclusion, compounds 4a , 8b, and 8g achieved the target goal. They elicited in vitro dual inhibition of COX-2/5-LOX higher than celecoxib and quercetin, in vivo potent anti-inflammatory activity higher than celecoxib and in vivo superior gastrointestinal safety profile (no ulceration) as celecoxib.

Published

2023

5. Rational design of biodegradable sulphonamide candidates treating septicaemia by synergistic dual inhibition of COX-2/PGE2 axis and DHPS enzyme.

Author

El-Dershaby NH, El-Hawash SA, Kassab SE, Dabees HG, Abdel Moneim AE, Abdel Wahab IA, Abd-Alhaseeb MM, and El-Miligy MMM

Subjects

Animals, Anti-Bacterial Agents pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Celecoxib adverse effects, Cyclooxygenase 2, Dinoprostone, Edema drug therapy, Mice, Sulfasalazine pharmacology, Sulfonamides pharmacology, Cyclooxygenase 2 Inhibitors pharmacology, Dihydropteroate Synthase antagonists & inhibitors, Enzyme Inhibitors pharmacology, Sepsis drug therapy

Abstract

A new series of co-drugs was designed based on hybridising the dihydropteroate synthase (DHPS) inhibitor sulphonamide scaffold with the COX-2 inhibitor salicylamide pharmacophore through biodegradable linkage to achieve compounds with synergistic dual inhibition of COX-2/PGE2 axis and DHPS enzyme to enhance antibacterial activity for treatment of septicaemia. Compounds 5 b, 5j, 5n and 5o demonstrated potent in vitro COX-2 inhibitory activity comparable to celecoxib. 5j and 5o exhibited ED 50 lower than celecoxib in carrageenan-induced paw edoema test with % PGE2 inhibition higher than celecoxib. Furthermore, 5 b , 5j and 5n showed gastric safety profile like celecoxib. Moreover, in vivo antibacterial screening revealed that, 5j showed activity against S.aureus and E.coli higher than sulfasalazine. While, 5o revealed activity against E.coli higher than sulfasalazine and against S.aureus comparable to sulfasalazine. Compound 5j achieved the target goal as potent inhibitor of COX-2/PGE2 axis and in vivo broad-spectrum antibacterial activity against induced septicaemia in mice.

Published

2022

6. Rational Design and Synthesis of New Selective COX-2 Inhibitors with In Vivo PGE2-Lowering Activity by Tethering Benzenesulfonamide and 1,2,3-Triazole Pharmacophores to Some NSAIDs.

Author

El-Dershaby NH, El-Hawash SA, Kassab SE, Daabees HG, Abdel Moneim AE, and El-Miligy MMM

Abstract

New selective COX-2 inhibitors were designed and synthesized by tethering 1,2,3-triazole and benzenesulfonamide pharmacophores to some NSAIDs. Compounds 6b and 6j showed higher in vitro COX-2 selectivity and inhibitory activity (IC 50 = 0.04 µM and S.I. = 329 and 312, respectively) than celecoxib (IC 50 = 0.05 µM and S.I. = 294). Compound 6e revealed equipotent in vitro COX-2 inhibitory activity to celecoxib. Furthermore, 6b and 6j expressed more potent relief of carrageenan-induced paw edema thickness in mice than celecoxib, with ED 50 values of 11.74 µmol/kg and 13.38 µmol/kg vs. 16.24 µmol/kg, respectively. Compounds 6b and 6j inhibited the production of PGE2 with a % inhibition of PGE2 production of 90.70% and 86.34%, respectively, exceeding celecoxib's percentage (78.62%). Moreover, 6b and 6j demonstrated a gastric safety profile comparable to celecoxib. In conclusion, compounds 6b and 6j better achieved the target goal as more potent and selective COX-2 inhibitors than celecoxib in vitro and in vivo.

Published

2022

7. Discovery of small molecule acting as multitarget inhibitor of colorectal cancer by simultaneous blocking of the key COX-2, 5-LOX and PIM-1 kinase enzymes.

Author

El-Miligy MMM, Al-Kubeisi AK, El-Zemity SR, Nassra RA, Abu-Serie MM, and Hazzaa AA

Subjects

Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents metabolism, Anti-Inflammatory Agents therapeutic use, Antineoplastic Agents metabolism, Antineoplastic Agents pharmacology, Apoptosis drug effects, Arachidonate 5-Lipoxygenase metabolism, Binding Sites, Catalytic Domain, Cell Line, Tumor, Colorectal Neoplasms pathology, Cyclooxygenase 2 metabolism, Drug Design, Edema chemically induced, Edema drug therapy, Edema pathology, Edema veterinary, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Humans, Molecular Docking Simulation, Proto-Oncogene Proteins c-pim-1 metabolism, Rats, Small Molecule Libraries metabolism, Small Molecule Libraries pharmacology, Small Molecule Libraries therapeutic use, Structure-Activity Relationship, Thiazolidines chemistry, Thiazolidines metabolism, Thiazolidines pharmacology, Thiazolidines therapeutic use, Antineoplastic Agents chemistry, Arachidonate 5-Lipoxygenase chemistry, Cyclooxygenase 2 chemistry, Enzyme Inhibitors chemistry, Proto-Oncogene Proteins c-pim-1 antagonists & inhibitors, Small Molecule Libraries chemistry

Abstract

Colorectal cancer (CRC) is the second cause of cancer death worldwide. Inhibitors of COX-2, 5-LOX and PIM-1 kinase were very effective in the treatment and prevention of CRC in mouse models in vivo. Furthermore, thymol was confirmed to inhibit CRC cell proliferation in cancer cell lines and inhibitory activity against COX-2 and 5-LOX. On the other hand, 4-thiazolidinone pharmacophore was incorporated in the structures of various reported COX-2, 5-LOX and PIM kinase inhibitors. Consequently, the aim of the present investigation was to combat CRC by synthesis and biological evaluation of new thymol - 4-thiazolidinone hybrids as multitarget anticancer agents that could inhibit the key COX-2, 5-LOX and PIM-1 kinase enzymes simultaneously. Compounds 5a-d and 5g displayed inhibitory activity against COX-2 nearly equal to Celecoxib with high selectivity index (SI). Moreover, compounds 5b-e showed 5-LOX inhibitory activity nearly equal to the reference Quercetin while compounds 5a, 5f and 5g elicited inhibitory activity slightly lower than Quercetin. Furthermore, in vivo formalin-induced paw edema test revealed that, compounds 5a, 5c, 5f and 5g showed higher % inhibition than Celecoxib and compounds 5a, 5f and 5g showed higher % inhibition than Diclofenac sodium. In addition, compounds 5a-c, 5e-g showed in vivo superior gastrointestinal safety profile as Celecoxib in fasted rats. Besides, compounds 5d, 5e and 5g exhibited the highest activity against human CRC cell lines (Caco-2 and HCT-116) at doses less than their EC 100 on normal human cells. Furthermore, compounds 5e and 5g induced apoptosis-dependent death by above 50% in the treated CRC cell lines. Moreover, compounds 5e and 5g induced caspase activation by >50% in human CRC. Also, compounds 5d, 5e and 5g showed in vitro inhibitory activity against both PIM-1\2 kinases comparable to the reference Staurosporine. In silico docking studies were concordant with the biological results. In conclusion, compound 5g, of simple chemical structure, achieved the target goal of inhibiting three targets leading to inhibition of human CRC cell proliferation. It inhibited the target key enzymes COX-2, 5-LOX and PIM-1\2 kinase in vitro. Besides, it revealed in vitro inhibition of cell proliferation in cancer cell lines via activation of caspase 3\7 dependent-apoptosis in human CRC cell lines. In addition, it elicited in vivo anti-inflammatory activity in formalin-induced paw edema test and in vivo oral safety in gastric ulcerogenic activity test., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

8. Design, synthesis and docking study of pyridine and thieno[2,3-b] pyridine derivatives as anticancer PIM-1 kinase inhibitors.

Author

Abdelaziz ME, El-Miligy MMM, Fahmy SM, Mahran MA, and Hazzaa AA

Subjects

Antineoplastic Agents chemical synthesis, Cell Line, Tumor, Drug Design, Drug Screening Assays, Antitumor, Humans, Molecular Docking Simulation, Neoplasms drug therapy, Neoplasms metabolism, Protein Kinase Inhibitors chemical synthesis, Proto-Oncogene Proteins c-pim-1 metabolism, Thienopyridines chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-pim-1 antagonists & inhibitors, Thienopyridines chemistry, Thienopyridines pharmacology

Abstract

A series of pyridine and thieno[2,3-b]pyridine derivatives have been designed and synthesized as anticancer PIM-1 kinase inhibitors. Thirty-seven compounds were selected by NCI to be tested initially at a single dose (10 µM) in the full NCI 60 cell line panel. Compound 5b showed potent anticancer activity and was tested twice in the five-dose assay which confirmed its potent antitumor activity (GI 50 values 0.302-3.57 µM) against all tested tumor cell lines except six cell lines where they showed moderate sensitivity. This compound was sent to NCI biological evaluation committee and still under consideration for further testing. In addition, the most active anticancer compounds in each series, 5b, 8d, 10c, 13h, and 15e, were evaluated for their PIM-1 kinase inhibitory activity. Compound 8d was the most potent one with IC 50  = 0.019 µM followed by 5b, 15e, 10c and 13h with IC 50 values 0.044, 0.083, 0.128 and 0.479 µM respectively. Moreover, docking study of the most active compounds in PIM-1 kinase active site was consistent with the in vitro activity., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

9. New hybrid molecules combining benzothiophene or benzofuran with rhodanine as dual COX-1/2 and 5-LOX inhibitors: Synthesis, biological evaluation and docking study.

Author

El-Miligy MMM, Hazzaa AA, El-Messmary H, Nassra RA, and El-Hawash SAM

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Anti-Inflammatory Agents, Non-Steroidal chemistry, Benzofurans chemistry, Benzofurans pharmacology, Catalytic Domain drug effects, Cyclooxygenase Inhibitors chemical synthesis, Cyclooxygenase Inhibitors chemistry, Dose-Response Relationship, Drug, Edema chemically induced, Edema drug therapy, Formaldehyde, Lipoxygenase Inhibitors chemical synthesis, Lipoxygenase Inhibitors chemistry, Male, Molecular Docking Simulation, Molecular Structure, Rats, Rats, Wistar, Rhodanine chemistry, Rhodanine pharmacology, Structure-Activity Relationship, Thiophenes chemistry, Thiophenes pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arachidonate 5-Lipoxygenase metabolism, Cyclooxygenase 1 metabolism, Cyclooxygenase 2 metabolism, Cyclooxygenase Inhibitors pharmacology, Lipoxygenase Inhibitors pharmacology

Abstract

New molecular hybrids combining benzothiophene or its bioisostere benzofuran with rhodanine were synthesized as potential dual COX-2/5-LOX inhibitors. The benzothiophene or benzofuran scaffold was linked at position -2 with rhodanine which was further linked to various anti-inflammatory pharmacophores so as to investigate the effect of such molecular variation on the anti-inflammatory activity. The target compounds were evaluated for their in vitro COX/LOX inhibitory activity. The results revealed that, compound 5h exhibited significant COX-2 inhibition higher than celecoxib. Furthermore, compounds 5a, 5f and 5i showed COX-2 inhibitory activity comparable to celecoxib. Compound 5h showed selectivity index SI=5.1 which was near to that of celecoxib (SI=6.7). Compound 5h displayed LOX inhibitory activity twice than that of meclofenamate sodium. Moreover, compounds 5a, 5e and 5f showed significant LOX inhibitory activity higher than that of meclofenamate sodium. Compound 5h was screened for its in vivo anti-inflammatory activity using formalin-induced paw edema and gastric ulcerogenic activity tests. The results revealed that, it showed in vivo decrease in formalin-induced paw edema volume higher than celecoxib. It also displayed gastrointestinal safety profile as celecoxib. The biological results were also consistent with the docking studies at the active sites of the target enzymes COX-2 and 5-LOX. Also, compound 5h showed physicochemical, ADMET, and drug-like properties within those considered adequate for a drug candidate., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017