Bioorganic Chemistry, Год журнала: 2020, Номер 96, С. 103575 - 103575
Опубликована: Янв. 10, 2020
Язык: Английский
Archiv der Pharmazie, Год журнала: 2021, Номер 355(1)
Опубликована: Сен. 24, 2021
Despite the advancements in development of anticancer agents, more effective and safer drugs still need to be developed as current agents cause unwanted side effects many patients have become drug resistant. 1,2,3-Triazoles, due their remarkable biological potential, received considerable attention discovery for agents. The present review article presents an overview recent advances 1,2,3-triazole hybrids with potential over last 2 years, chemical structures, structure-activity relationships, mechanisms action, well insights into docking studies.
Язык: Английский
Процитировано
214
European Journal of Medicinal Chemistry, Год журнала: 2024, Номер 270, С. 116363 - 116363
Опубликована: Март 29, 2024
Язык: Английский
Процитировано
23
Medicinal Research Reviews, Год журнала: 2023, Номер 43(5), С. 1778 - 1808
Опубликована: Май 14, 2023
Abstract The antitumor efficacy of Chinese herbal medicines has been widely recognized. Leading compounds such as sterols, glycosides, flavonoids, alkaloids, terpenoids, phenylpropanoids, and polyketides constitute their complex active components. monomers derived from medicine possess an attractive anticancer activity. However, use was limited by low bioavailability, significant toxicity, side effects, hindering clinical applications. Recently, new chemical entities have designed synthesized combining natural drugs with other small drug molecules or moieties to improve the activity selectivity, reduce effects. Such a novel conjugated that can interact several vital biological targets in cells may more synergistic than single‐molecule drug. In addition, conjugates could be obtained pharmacophores containing two known leading compounds. Based on these studies, research development greatly shortened. This study reviews progress based medicine. It is expected serve valuable reference application traditional
Язык: Английский
Процитировано
37
European Journal of Medicinal Chemistry, Год журнала: 2024, Номер 274, С. 116535 - 116535
Опубликована: Май 31, 2024
Язык: Английский
Процитировано
12
International Journal of Biological Macromolecules, Год журнала: 2025, Номер 297, С. 139885 - 139885
Опубликована: Янв. 14, 2025
Язык: Английский
Процитировано
1
European Journal of Medicinal Chemistry, Год журнала: 2020, Номер 210, С. 112954 - 112954
Опубликована: Окт. 30, 2020
Язык: Английский
Процитировано
59
Journal of Molecular Structure, Год журнала: 2020, Номер 1209, С. 127951 - 127951
Опубликована: Фев. 22, 2020
Язык: Английский
Процитировано
55
Food Chemistry, Год журнала: 2022, Номер 387, С. 132938 - 132938
Опубликована: Апрель 9, 2022
Язык: Английский
Процитировано
33
Journal of Medicinal Chemistry, Год журнала: 2023, Номер 66(2), С. 1426 - 1453
Опубликована: Янв. 17, 2023
A novel, potent, and selective antitumor agent, namely (E)-3-phenyl-1-(2-pyridinyl)-2-propen-1-one 4,4-dimethyl-3-thiosemicarbazone (PPP44mT), its analogues were synthesized characterized displayed strikingly distinctive properties. This activity was mediated by the inclusion of a styrene moiety, which through steric electrochemical mechanisms prevented deleterious oxy-myoglobin or oxy-hemoglobin oxidation relative to other potent thiosemicarbazones, i.e., di-2-pyridylketone-4-cyclohexyl-4-methyl-3-thiosemicarbazone (DpC) di-2-pyridylketone-4,4-dimethyl-3-thiosemicarbazone (Dp44mT). Structure–activity relationship analysis demonstrated specific tuning PPP44mT electrochemistry further inhibited oxidation. Both Cu(II) complexes showed conspicuous almost immediate cytotoxicity against SK-N-MC tumor cells (within 3 h). In contrast, [Zn(PPP44mT)2] pronounced delay in activity, taking 48 h before marked antiproliferative efficacy apparent. As such, designated as "stealth Zn(II) complex" that overcomes near copper complexes. Upon examination suppression oncogenic signaling, superior at inhibiting cyclin D1 expression compared DpC Dp44mT.
Язык: Английский
Процитировано
19
Dalton Transactions, Год журнала: 2023, Номер 52(15), С. 4737 - 4751
Опубликована: Янв. 1, 2023
Twenty new zinc(II) complexes with 8-hydroxyquinoline (H-Q1-H-Q6) in the presence of 1,10-phenanthroline derivatives (D1-D10) were synthesized and formulated as [Zn(Q1)2(D1)] (DQ1), [Zn(Q2)2(D2)]·CH3OH (DQ2), [Zn(Q1)2(D3)] (DQ3), [Zn(Q1)2(D4)] (DQ4), [Zn(Q3)2(D5)] (DQ5), [Zn(Q3)2(D4)] (DQ6), [Zn(Q4)2(D5)]·CH3OH (DQ7), [Zn(Q4)2(D6)] (DQ8), [Zn(Q4)2(D3)]·CH3OH (DQ9), [Zn(Q4)2(D1)]·H2O (DQ10), [Zn(Q5)2(D4)] (DQ11), [Zn(Q6)2(D6)]·CH3OH (DQ12), [Zn(Q5)2(D2)]·5CH3OH·H2O (DQ13), [Zn(Q5)2(D7)]·CH3OH (DQ14), [Zn(Q5)2(D8)]·CH2Cl2 (DQ15), [Zn(Q5)2(D9)] (DQ16), [Zn(Q5)2(D1)] (DQ17), [Zn(Q5)2(D5)] (DQ18), [Zn(Q5)2(D10)]·CH2Cl2 (DQ19) [Zn(Q5)2(D3)] (DQ20). They characterized using multiple techniques. The cytotoxicity DQ1-DQ20 was screened human cisplatin-resistant SK-OV-3/DDP ovarian cancer (SK-OV-3CR) cells normal hepatocyte (HL-7702) cells. Complex DQ6 showed low IC50 values (2.25 ± 0.13 μM) on SK-OV-3CR cells, more than 3.0-8.0 times cytotoxic DQ1-DQ5 DQ7-DQ20 (≥6.78 μM), even 22.2 standard cisplatin, corresponding free H-Q1-H-Q6 D1-D10 alone (>50 μM). As a comparison, displayed nontoxic rates against healthy HL-7702 Furthermore, DQ11 induced significant apoptosis via mitophagy pathways. also significantly inhibited tumor growth an vivo SK-OV-3-xenograft model (ca. 49.7%). Thus, may serve lead complex for discovery antitumor agents.
Язык: Английский
Процитировано
18