Comparison of Free‐Hydroxy With 3′,5′‐Di‐O‐Acetyl Ribose of 5‐Alkynyl Dicobalt Hexacarbonyl 2′‐Deoxy‐Furopyrimidines Hybrids: Synthesis, Antiproliferative Activity, and ROS Determination

Author:

Kaczmarek Renata1ORCID,Radzikowska‐Cieciura Ewa1ORCID,Królewska‐Golińska Karolina1ORCID,Andrei Graciela2ORCID,Snoeck Robert2ORCID,Dolot Rafał1ORCID,Wheeler Kraig A.3ORCID,Agyei Gyimah Dominic4ORCID,Yang Susan4ORCID,Dembinski Roman14ORCID

Affiliation:

1. Centre of Molecular and Macromolecular Studies Polish Academy of Sciences Łódź Poland

2. Department of Microbiology, Immunology and Transplantation Rega Institute Leuven Belgium

3. Department of Chemistry Whitworth University Spokane Washington USA

4. Department of Chemistry Oakland University Rochester Michigan USA

Abstract

ABSTRACTSynthesis of 5‐alkynyl furopyrimidine nucleoside analogs, with free‐ribose groups, was carried out, and their biological activity was evaluated. The substituents introduced at the C‐5 included propargyl and homopropargyl alcohols, 4‐methylphenyl (p‐tolyl), and 4‐pentylphenyl substituted alkynyl groups (56%–88%). Subsequently, alkyne function was coordinated to dicobalt hexacarbonyl unit, yielding the corresponding dicobalt hexacarbonyl 5‐alkynyl furopyrimidine nucleosides (51%–75%). All compounds contained 4‐pentylphenyl group attached at the C‐6 position of the bicyclic base, in line with most active antiviral structures. The antiproliferative effect of these modified nucleosides on cancer cells of different phenotypes was determined using in vitro studies. The tested compounds show antiproliferative effects with median inhibitory concentration (IC50) values of 16–23 and 9–15 μM for HeLa and K562 cells, respectively. The determination of reactive oxygen species (ROS) formation in K562 cells in the presence of modified nucleosides may suggest that the mode of action of the examined compounds may be attributed to the induction of oxidative stress.

Funder

National Institutes of Health

National Science Foundation

Publisher

Wiley

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