A Facile One‐Pot Synthesis of New Fused Indole Pyrazole Derivatives and Their Anticancer and Antidiabetic Activities DOI Creative Commons
Senzekile Majola, Myalowenkosi I. Sabela, Robert Moonsamy Gengan

et al.

ChemistrySelect, Journal Year: 2024, Volume and Issue: 9(48)

Published: Dec. 1, 2024

Abstract Indole‐pyrazole hybrids are intriguing due to their potential for synergistic pharmacological effects, unlike molecules with only one pharmacophore. This study presents a one‐pot synthesis of fused indole‐pyrazole derivatives, bis 4a and chromone 4b using an aldehyde, thiosemicarbizide, indole, as anticancer antidiabetic agents. The synthesized compounds were characterized Fourier transform infrared (FTIR), nuclear magnetic resonance (NMR), time‐of‐flight mass spectrometry (TOF‐MS). Initially, mutagenicity test was performed, the showed no significant increase in revertant colonies against Salmonella typhimurium TA 98 100 strains. In MTT assay cytotoxicity two human cancer cell lines, A549 HepG‐2; normal line, HEK 293. Compound high potency IC 50 values 18.70 50.07 µg/mL, respectively, whereas both low inhibition level 293 at µg/mL. vitro α‐amylase α‐glucosidase, compound demonstrated excellent 3.9 µg/mL 12.1 respectively.

Language: Английский

Fluorinated indeno-quinoxaline bearing thiazole moieties as hypoglycaemic agents targeting α -amylase, and α -glucosidase: synthesis, molecular docking, and ADMET studies DOI Creative Commons

Nirvana A. Gohar,

Eman A. Fayed, Yousry A. Ammar

et al.

Journal of Enzyme Inhibition and Medicinal Chemistry, Journal Year: 2024, Volume and Issue: 39(1)

Published: June 24, 2024

Inhibition of α-glucosidase and α-amylase are key tactics for managing blood glucose levels. Currently, stronger, more accessible inhibitors needed to treat diabetes. Indeno[1,2-b] quinoxalines-carrying thiazole hybrids 1–17 were created described using NMR. All analogues tested hypoglycaemic effect against STZ-induced diabetes in mice. Compounds 4, 6, 8, 16 the most potent among synthesised analogues. These examined their effects on plasma insulin, urea, creatinine, GSH, MDA, ALT, AST, total cholesterol. Moreover, these compounds enzymes vitro. The four represented moderate activity with IC50 values 0.982 ± 0.04, 10.19 0.21 inhibition 17.58 0.74 121.6 5.14 μM when compared standard medication acarbose IC50=0.316 0.02 31.56 1.33 inhibition. Docking studies as well silico ADMT done.

Language: Английский

Citations

12
Synthesis, design, biological evaluation, and computational analysis of some novel uracil-azole derivatives as cytotoxic agents DOI Creative Commons
Leila Emami, Fatemeh Zare, Soghra Khabnadideh

et al.

BMC Chemistry, Journal Year: 2024, Volume and Issue: 18(1)

Published: Jan. 3, 2024

Abstract The design and synthesis of novel cytotoxic agents is still an interesting topic for medicinal chemistry researchers due to the unwanted side effects anticancer drugs. In this study, a series uracil–azole hybrids were designed synthesized. activity, along with computational studies: molecular docking, dynamic simulation, density functional theory, ADME properties also, evaluated. compounds synthesized by using 3-methyl-6-chlorouracil as starting material. Cytotoxicity was determined MTT assay in breast carcinoma cell line (MCF-7) Hepatocellular (HEPG-2). These derivatives demonstrated powerful inhibitory activity against hepatocellular lines comparison Cisplatin positive control. Among these compounds, 4j displayed best selectivity profile good IC 50 values 16.18 ± 1.02 7.56 5.28 µM MCF-7 HEPG-2 respectively. Structure–activity relationships revealed that variation potency affected various substitutions benzyl moiety. docking output showed bind well active site EGFR formed stable complex protein. DFT used investigate reactivity descriptors 4a . outputs can be considered potential agents.

Language: Английский

Citations

8
Fluorinated thiazole–thiosemicarbazones hybrids as potential PPAR-γ agonist and α-amylase, α-glucosidase antagonists: Design, synthesis, in silico ADMET and docking studies and hypoglycemic evaluation DOI
Eman A. Fayed,

Aya Thabet,

Shimaa M. Abd El‐Gilil

et al.

Journal of Molecular Structure, Journal Year: 2023, Volume and Issue: 1301, P. 137374 - 137374

Published: Dec. 21, 2023

Language: Английский

Citations

16
Novel Pyrrolidine-bearing quinoxaline inhibitors of DNA Gyrase, RNA polymerase and spike glycoprotein DOI

Maha A. Ebrahim,

Triveena M. Ramsis,

Nirvana A. Gohar

et al.

Bioorganic Chemistry, Journal Year: 2025, Volume and Issue: 156, P. 108218 - 108218

Published: Jan. 27, 2025

Language: Английский

Citations

0
Novel 3‐Substituted‐2H‐Chromene Scaffold Based Fluorinated Hydrophobic Fragment as In‐Vitro Antiproliferative Agents and Apoptosis Inducers Targeting Both VEGFR‐2/BRAFV600E and h‐DHFR With Molecular Docking Simulation DOI Open Access
Mohamed A. Salem,

Moustafa S. Abusaif,

Nirvana A. Gohar

et al.

Drug Development Research, Journal Year: 2025, Volume and Issue: 86(2)

Published: March 28, 2025

ABSTRACT Recently, there has been an increasing interest in the use of protein kinase inhibitors as a therapeutic strategy for treatment cancer. In this study, new series 2 H ‐chromene derivatives ( ‐ 5 and 6 8 ) 3 ‐benzo[ f ]chromene carbohydrazide derivative 9 were synthesized. The structure designed was characterized by IR, 1 H/ 13 C NMR, elemental analysis. Moreover, cytotoxic activity newly synthesized chromenes evaluated against breast cancer cell lines (MDA‐MB‐231 MCF‐7) cervical line (HeLa). results these evaluations demonstrated promising activity, ranging from good to moderate. Additionally, lung fibroblast (WI‐38), normal line, also utilized assess active derivatives' selectivity. Among compounds tested, chromene highest potency, exhibiting IC 50 values 5.36 ± 0.50, 7.82 0.60, 9.28 0.70 µM MDA‐MB 231, MCF‐7, HeLa lines, respectively. potential chromone multi‐targeted anticancer agent assessed evaluating its BRAF VEGFR‐2. Notably, most significant VEGFR2 with value 0.224 compared sorafenib's 0.045 µM, while inhibitory 1.695 relative Vemurafenib's 0.468 µM. addition, compound inhibits DHFR enzyme 2.217 0.014 methotrexate (IC = 0.4315 0.019 µM). These revealed that multifaceted mechanisms action may augment effectiveness. causes overexpression caspase‐3 Bax 6.13 8.85‐fold, It downregulates antiapoptotic Bcl‐2 level 0.4775‐fold untreated 231 cells. Flow cytometry analysis MDA‐MB‐231 cells indicates induces cycle arrest G0‐G1 phase, observed percentage 73.15%. in‐silico toxicity prediction profile. Finally, molecular docking studies supported findings confirming strong binding affinities VEGFR‐2, BRAF, DHFR.

Language: Английский

Citations

0
Exploring a novel thiazole derivatives hybrid with fluorinated-indenoquinoxaline as dual inhibitors targeting VEGFR2/AKT and apoptosis inducers against hepatocellular carcinoma with docking simulation DOI

Moustafa S. Abusaif,

Ahmed Ragab, Eman A. Fayed

et al.

Bioorganic Chemistry, Journal Year: 2024, Volume and Issue: 154, P. 108023 - 108023

Published: Dec. 2, 2024

Language: Английский

Citations

3
Pyrano-coumarin hybrids as potential antimicrobial agents against MRSA strains: Design, synthesis, ADMET, molecular docking studies, as DNA gyrase inhibitors DOI
Eman A. Fayed,

Maha A. Ebrahim,

Usama Fathy

et al.

Journal of Molecular Structure, Journal Year: 2023, Volume and Issue: 1295, P. 136663 - 136663

Published: Sept. 17, 2023

Language: Английский

Citations

8
Design, synthesis, biological evaluation and molecular docking study of new pyrazolo[1,5-a]pyrimidines as PIM kinase inhibitors and apoptosis inducers DOI
Fatma G. Abdulrahman, Rehab Sabour, Shimaa M. Abd El‐Gilil

et al.

Journal of Molecular Structure, Journal Year: 2023, Volume and Issue: 1295, P. 136811 - 136811

Published: Oct. 9, 2023

Language: Английский

Citations

8
Novel uracil derivatives as anti-cancer agents: Design, synthesis, biological evaluation and computational studies DOI

Ladan Baziyar,

Parinaz Ahmadi,

Saman Zare Gheshlaghi

et al.

Journal of Molecular Structure, Journal Year: 2023, Volume and Issue: 1302, P. 137435 - 137435

Published: Dec. 27, 2023

Language: Английский

Citations

4
Discovery of Novel Bicyclic and Tricyclic Cyclohepta[b]thiophene Derivatives as Multipotent AChE and BChE Inhibitors, In-Vivo and In-Vitro Assays, ADMET and Molecular Docking Simulation DOI Creative Commons
Eman A. Fayed, Samiha A. El‐Sebaey,

Maha A. Ebrahim

et al.

European Journal of Medicinal Chemistry, Journal Year: 2024, Volume and Issue: 284, P. 117201 - 117201

Published: Dec. 24, 2024

Language: Английский

Citations

1