Azafuramidines as Potential Anticancer Agents: Pro-apoptotic Profile and Cell Cycle Arrest

Elsibaei, Sameh M; Amleh, Asma; Ismail, Mohamed A; El-Sayed, Wael;

Abstract


The current study aimed to test the antiproliferative activity of three azafuramidines (X, Y, and Z) against three different human cell lines; liver HepG2, breast MCF-7, and bone U2OS. And to explore the molecular mechanism(s) of the antiproliferative activity of these derivatives. The three new azafuramidines demonstrated a potent cytotoxicity at < 2 μM against the three cell lines investigated. The azafuramidines were highly selective with selectivity index ∼ 47 - 61 folds indicating safety to the normal cells. In the scratch assay, azafuramidines significantly reduced the percentage of wound healing indicating ability to prevent or reduce metastasis. Derivatives X and Z arrested the HepG2 cells at S and G2/M phases detected by the flow cytometry. Derivatives X, Y, and Z elevated the apoptosis of HepG2 cells by ∼71%, 66%, and 59%, respectively. Derivatives X and Z were superior to derivative Y. The potent antiproliferative, cell cycle arrest, and pro-apoptotic efficacy of these chlorophenyl derivatives could be attributed to their ability of inducing the overexpression of p53, p21, and p27. These derivatives had the potential to act as anticancer agents. and merit further investigations.


Other data

Title Azafuramidines as Potential Anticancer Agents: Pro-apoptotic Profile and Cell Cycle Arrest
Authors Elsibaei, Sameh M; Amleh, Asma ; Ismail, Mohamed A ; El-Sayed, Wael 
Keywords Apoptosis;Cell cycle;Flow cytometry;Scratch assay;p21;p53
Issue Date 10-Nov-2023
Journal Bioorganic & medicinal chemistry letters 
Volume 97
ISSN 0960894X
DOI 10.1016/j.bmcl.2023.129550
PubMed ID 37952598

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