Discovery of novel potent human chondrosarcoma (SW1353) inhibitors: 4-(2/3/4-pyridyl)thiazole 2-acetamide derivatives

•24 novel thiazole derivatives were synthesized.•Chondrosarcoma inhibitors are discovered.•Apoptotic pathways are monitorized.•Tyrosine kinases could be the key macromolecules for chondrosarcoma. Chondrosarcoma is the most common cartilage sarcoma among adult patients. It is mainly observed after th...

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Bibliographic Details
Published in:Journal of molecular structure 2023-02, Vol.1273, p.134260, Article 134260
Main Authors: Coşkun, Göknil Pelin, Sahin, Zafer, Erdoğan, Ömer, Çevik, Özge, Biltekin, Sevde Nur, Yurttas, Leyla, Berk, Barkin, Ülgen, Mert, Demirayak, Şeref
Format: Article
Language:English
Subjects:
Amide
Antitumor
Apoptosis
Chondrosarcoma
Kinase
SW1357
Thiazole
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Summary:•24 novel thiazole derivatives were synthesized.•Chondrosarcoma inhibitors are discovered.•Apoptotic pathways are monitorized.•Tyrosine kinases could be the key macromolecules for chondrosarcoma. Chondrosarcoma is the most common cartilage sarcoma among adult patients. It is mainly observed after the degradation of chondrocytes in the case of cell stress. Unfortunately, the mortality among patients is high as a result of metastasis. Here in this study we have discovered some novel 4-(2/3/4-pyridyl)thiazole2-acetamide derivatives and elucidated their structure using chromatographic and spectroscopic methods. The antitumor activity profile for the synthesized compounds was performed using an MTT assay and apoptotic pathways (BAX, BCL-2) on the chondrosarcoma (SW1353) cell line. Besides, tyrosine kinase activity studies were also performed in order to understand the underlying mechanism of action. Among the synthesized compounds, there are some compounds showed excellent activity on chondrosarcoma cells. Besides, compounds showed no cytotoxicity on healthy fibroblast (L929) cell lines. Among the compounds, the compound having benzimidazole moiety showed the highest activity with IC50 value of 2.03±1.05 µM compared to doxorubicin (5.05±1.07 µM). The results indicated that the anticancer activity of the compounds might be depending on tyrosine kinase inhibiton. The compounds are also exhibited to induce apoptosis in chondrosarcoma cells. Morphological and colony observations are also successfully visualized. [Display omitted]
ISSN:0022-2860
1872-8014
DOI:10.1016/j.molstruc.2022.134260