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dc.contributor.authorChawannuch Mudjupaen_US
dc.contributor.authorSewan Theeramunkongen_US
dc.contributor.authorOpa Vajraguptaen_US
dc.date.accessioned2019-05-07T09:59:37Z-
dc.date.available2019-05-07T09:59:37Z-
dc.date.issued2017en_US
dc.identifier.issn0125-2526en_US
dc.identifier.urihttp://it.science.cmu.ac.th/ejournal/dl.php?journal_id=8036en_US
dc.identifier.urihttp://cmuir.cmu.ac.th/jspui/handle/6653943832/63896-
dc.description.abstractNovel caffeic acid amides were designed and evaluated for their antiproliferative activities against a panel of tumor cell lines. The development based on the caffeic core structure of the identified hit compound from virtual screening of 2,666 compounds against tyrosine kinase receptor. The compounds were designed by using amide to link the caffeic core with the privileged motif, thiazole via target-based approach. Molecular docking studies indicated that the designed compounds were nicely bound to the EGFR tyrosine kinase. Among the synthesized compounds, CAD1 and CAD2 exhibited potent antiproliferative activity against breast cancer MCF-7 cells with IC50 of 8.02 and 13.69 mM, respectively. The molecular mechanism was investigated and found that CAD1 and CAD2 induced cell death by apoptosis and inhibited EGFR kinase.en_US
dc.languageEngen_US
dc.publisherScience Faculty of Chiang Mai Universityen_US
dc.titleDesign and Synthesis of Caffeic Amides by Structure-based Approachesen_US
dc.typeบทความวารสารen_US
article.title.sourcetitleChiang Mai Journal of Scienceen_US
article.volume44en_US
article.stream.affiliationsCenter of Excellence for Innovation in Drug Design and Discovery, Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Mahidol University, 447 Sri-Ayudhya Road, Bangkok 10400, Thailand.en_US
article.stream.affiliationsFaculty of Pharmacy, Mahasarakham University, Kantarawichai District, Maha Sarakham, Thailand 44150, Thailand.en_US
article.stream.affiliationsFaculty of Pharmacy, Thammasat University, 99 Moo 18 Phahonyothin Road, Klongluang, Pathumthani, Thailand, 12120.en_US
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