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Furo[2,3‐<i>d</i>]pyrimidines as Mackinazolinone/Isaindigotone Analogs: Synthesis, Modification, Antitumor Activity, and Molecular Docking Study

Buer SongState Key Laboratory Basis of Xinjiang Indigenous Medicinal Plants Resource Utilization Xinjiang Technical Institute of Physics and Chemistry Chinese Academy of Sciences South Beijing Rd 40–1 Urumqi 830011 P. R. ChinaLifei NieState Key Laboratory Basis of Xinjiang Indigenous Medicinal Plants Resource Utilization Xinjiang Technical Institute of Physics and Chemistry Chinese Academy of Sciences South Beijing Rd 40–1 Urumqi 830011 P. R. ChinaKhurshed BozorovFaculty of Chemistry Samarkand State University University Blvd. 15 Samarkand 140104 UzbekistanChao NiuState Key Laboratory Basis of Xinjiang Indigenous Medicinal Plants Resource Utilization Xinjiang Technical Institute of Physics and Chemistry Chinese Academy of Sciences South Beijing Rd 40–1 Urumqi 830011 P. R. ChinaRustamkhon KuryazovFaculty of Chemistry Samarkand State University University Blvd. 15 Samarkand 140104 UzbekistanHaji Akber AisaState Key Laboratory Basis of Xinjiang Indigenous Medicinal Plants Resource Utilization Xinjiang Technical Institute of Physics and Chemistry Chinese Academy of Sciences South Beijing Rd 40–1 Urumqi 830011 P. R. ChinaJiangyu ZhaoState Key Laboratory Basis of Xinjiang Indigenous Medicinal Plants Resource Utilization Xinjiang Technical Institute of Physics and Chemistry Chinese Academy of Sciences South Beijing Rd 40–1 Urumqi 830011 P. R. China
Chemistry & Biodiversityjournal2023en
ABI

Аннотация

Abstract The chemical transformation of the tricyclic furo[2,3‐ d ]pyrimidines was performed under isosteric and scaffold‐hopping strategies focusing on the synthesis of its arylidene and imine‐containing derivatives. Naturally‐occurring alkaloids mackinazolinone and isaindigotone were as templates of target heterocycles. Synthesized compounds evaluated for their antitumor activity on human cancer cervical HeLa, breast MCF‐7, and colon HT‐29 cell lines. Four compounds: 8c , 8e , 10b , and 10c demonstrated potency against HeLa and HT‐29 cell lines, and IC 50 values were between 7.37–13.72 μM, respectively. The molecular docking results showed that compounds 8c and 10b had good binding and high matching with the target EGFR protein.

Мавзулар

Quinazolinone synthesis and applicationsCancer therapeutics and mechanismsSynthesis and Biological Evaluation

Идентификаторлар

DOI
10.1002/cbdv.202201059

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