Chitosan functionalized thiophene-2-thiosemicarbazones, and their copper(II) complexes: synthesis, characterization, and anticancer activity

被引:15
|
作者
Adhikari, Hari Sharan [1 ]
Garai, Aditya [2 ]
Thapa, Machchhendra [3 ]
Adhikari, Rameshwar [4 ,5 ]
Yadav, Paras Nath [4 ]
机构
[1] Tribhuvan Univ, Inst Engn, Dept Appl Sci, Pashchimanchal Campus, Pokhara, Nepal
[2] Indian Inst Sci, Dept Inorgan & Phys Chem, Bangalore, Karnataka, India
[3] Tribhuvan Univ, Cent Dept Biotechnol, Kathmandu, Nepal
[4] Tribhuvan Univ, Cent Dept Chem, Kathmandu 44600, Nepal
[5] Tribhuvan Univ, Res Ctr Appl Sci & Technol RECAST, Kathmandu, Nepal
关键词
Anticancer activity; characterization; chitosan; chitosan thiophene-2-thiosemicarbazones; copper(II) chitosan thiophene-2-thiosemicarbazones; thiophene-2-carboxaldehyde; PALLADIUM(II) COMPLEXES; BIOLOGICAL-ACTIVITY; IN-VITRO; CRYSTAL-STRUCTURE; BREAST-CANCER; THIOPHENE-2-CARBALDEHYDE THIOSEMICARBAZONE; STRUCTURAL-CHARACTERIZATION; ANTIBACTERIAL ACTIVITY; MOLECULAR ASSOCIATION; THIOPHENE DERIVATIVES;
D O I
10.1080/10601325.2021.2022982
中图分类号
O63 [高分子化学(高聚物)];
学科分类号
070305 ; 080501 ; 081704 ;
摘要
Chitosan is a polyfunctional biomaterial that is subjected to chemical modification through functionalization to give the derivatives of remarkable anticancer activity. In this study, functionalization of low molecular weight commercial chitosan (CS) (Mw < 3000 Da, 87% DDA) and high molecular weight crab shell chitosan (CCS) (viscosity average Mw 350 kDa, 67% DDA) as chitosan thiophene-2-thiosemicarbazones (DS 63.48-64.14%) and the formation of their copper(II) complexes were established by FT-IR, C-13 NMR, EPR spectroscopy, powder X ray diffraction, elemental microanalysis and magnetic susceptibility measurements. The thermal study of the compounds showed a substantial stability up to 200 degrees C until the commencement of chitosan chain degradation. The MTT assay revealed higher activity of CS (IC50 370 mu gmL(-1) in MCF-7 and >400 mu gmL(-1) in MDCK cell line) than CCS (IC50 > 400 mu gmL(-1) in both cell lines), higher activity of CSTHPTSC (IC50 364 mu gmL(-1) in MDCK and 369 mu gmL(-1) in MCF-7 cell line) than CCSTHPTSC (IC50 > 400 mu gmL(-1) in both cell lines), higher activity of the complexes Cu-CSTHPTSC (IC50 338 mu gmL(-1) in MDCK and 318 mu gmL(-1) in MCF-7 cell line) and Cu-CCSTHPTSC (IC50 293 mu gmL(-1) in MDCK and >400 mu gmL(-1) in MCF-7 cell line) than their corresponding ligands.
引用
收藏
页码:211 / 227
页数:17
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