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Research Articles

Facile synthesis and cytotoxicity of substituted uracil-1'(N)-acetic acid and 4-pyridone-1'(N)-acetic acid esters of 20(S)-camptothecins

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Pages 259-268 | Received 15 Sep 2023, Accepted 25 Dec 2023, Published online: 12 Feb 2024
 

Abstract

A series of novel substituted uracil-1'(N)-acetic acid esters (59) and 4-pyridone-1'(N)-acetic acid esters (1011) of 20(S)-camptothecins (CPTs) have been synthesized by the acylation method. All of these new esters were assayed for in vitro cytotoxicity against five human cancer cell lines A549, Bel7402, BGC-823, HCT-8 and A2780. The in vitro bioassay results showed that all the synthesized compounds 511 had cytotoxities that were higher than TPT and comparable to CPT on these five tumor cell lines, some of them even showed comparable or superior cytotoxic activity to CPT. The in vitro data exhibited the cytotoxicity of the ester depended on that of its parent compound. The ester 5, 6, 8, 10, 11 even possessed the cytotoxity activity comparable to or even a little better than CPT on A549, HCT-8 and A2780. The compound 11 had the same level of cytoxity on Bel7402 as that of CPT. Here the synthesis and the in vitro antitumor evaluation of a series of novel 20-O-linked substituted uracil-1'(N)-acetic acid and 4-pyridone-1'(N)-acetic acid esters derivatives of CPTs are reported.

Disclosure statement

No potential conflict of interest was reported by the author(s).

Additional information

Funding

This study was financially supported in part by “National Key R&D Program of China [Grant No. 2022YFC3500105],” “the Fundamental Research Funds for the Central Universities [No. 2020-JYB-XJSJJ-005]” and “the major projects in Ordos [No. 2021ZD she30-22]”.

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