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n-(4-(4-chlorophenyl)thiazol-2-yl)-2-(2-phenylacetamido) acetamide derivatives as potential anticancer agents: synthesis and cytotoxicity evaluation
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نویسنده
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aliabadi alireza ,mohammadi-farani ahmad ,hosseini amin ,nikray semko ,foroumadi ali reza ,aliabadi amin
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منبع
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iranian journal of chemistry and chemical engineering - 2024 - دوره : 43 - شماره : 6 - صفحه:2188 -2202
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چکیده
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According to the rising statistics of cancer cases, the discovery of novel anticancer drugs is a critical issue in current medical research. besides, drug resistance and the incidence of severe adverse effects are the logical reasons for the discovery of new antineoplastic agents. according to the positive background that has been observed for 1,3-thiazole derivatives as potential anticancer drugs, we decided to synthesize a new series of 1,3-thiazole-based cytotoxic agents. mtt assay, activation of caspase 3, capability for reduction of the mitochondrial membrane potential (mmp), and production potency of reactive oxygen species (ros) were investigated. some of the tested compounds demonstrated potent cytotoxic activity and also caspase 3 activation, mmp reduction, and ros generation. three cancerous cell lines namely hela (cervical cancer), a549 (lung carcinoma), and u87 (glioblastoma) were applied to perform the mtt assay. diverse moieties with different electronic features were substituted on the phenyl ring to reveal the structure-activity relationships of the target compounds 8a-8o. hela (cervical cancer), a549 (lung carcinoma), and u87 (glioblastoma) were utilized as cancerous cells to explore the cytotoxicity via mtt hela and u87 cells were more sensitive to the tested compounds and a549 was more resistant to the tested derivatives. compound 8a with ortho chlorine moiety on the phenyl ring was the most active derivative against hela cells (ic50 = 1.3±0.14 µm). all evaluated derivatives rendered lower activity against a549 than doxorubicin as a standard anticancer drug. only some of the evaluated compounds showed more cytotoxicity against u87 than doxorubicin. furthermore, caspase 3 activation, mitochondrial membrane potential (mmp), and reactive oxygen species (ros) generation were also investigated. fortunately, some of the tested compounds were also active in these tests. in conclusion, the current 1,3-thiazole derivatives could be suggested as potential anticancer lead compounds.
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کلیدواژه
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synthesis ,3-thiazole ,phenylacetamide ,cytotoxicity ,caspase 3
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آدرس
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kermanshah university of medical sciences, faculty of pharmacy, department of medicinal chemistry, iran, shahrekord university of medical sciences, medical plants research center, basic health sciences institute, iran, kermanshah university of medical sciences, students research committee, iran, kermanshah university of medical sciences, students research committee, iran, tehran university of medical sciences, faculty of pharmacy and pharmaceutical sciences research center, department of medicinal chemistry, iran, shiraz university of medical sciences, school of medicine, department of pharmacology, iran
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پست الکترونیکی
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aliabadi.amin@gmail.com
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Authors
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