JOURNAL OF BIOLOGY AND GENETIC RESEARCH (JBGR )

E-ISSN 2545-5710
P-ISSN 2695-222X
VOL. 10 NO. 1 2024
DOI: https://doi.org/10.56201/jbgr.v10.no1.2024.pg32.41


Estimation of Antiproliferative Activity of Modified Thio- Nucleosides on MCF-7 Cells Line

S.Albasri, A.G. Sysa, E.I. Kvasyuk, E.R. Gritskevich


Abstract


The MCF-7 cell line, a well-researched human breast cancer model, has significantly contributed to advancing our knowledge of breast cancer biology and innovating treatment approaches. A notable trait of MCF-7 cells is their responsiveness to estrogen. Research involving MCF-7 cells has yielded significant knowledge regarding hormone receptor signaling and the modes of operation of anti-estrogen treatments like tamoxifen. Furthermore, MCF-7 cells have served as a platform for investigating drug resistance and for identifying prospective anti-cancer agents[1]. Modified nitrogen bases 2-mercaptopurine, thioguanine, and nucleosides 6-thioguanosine and 2’-deoxy-6-thioguanosine, along with Desulfated_Aztreonam and 2-(Benzylsulfanyl)-1-hydroxyadenosine, were evaluated for their potential anticancer properties. The antiproliferative assay was utilized to examine the characteristics of MCF-7 cells. The findings indicated that 2-mercaptopurine exhibited notable efficacy against MCF-7 cells, resulting in a 40% inhibition of growth[4]. Treatment with nitrogen bases 2-mercaptopurine and 6-thioguanine, along with nucleosides 6-thioguanosine and 2’-deoxy-6-thioguanosine, may exhibit antibacterial properties against MCF-7. Our findings offer fresh perspectives on the cytotoxic efficacy of thiopurines and propose a justification for opting for mercaptopurine over thioguanine in addressing various bacterial- induced illnesses.


keywords:

MCF-7; anticancer activity; antibacterial activity; thionucleosides


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