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Design and Synthesis of New Dihydropyrimidine Derivatives with a Cytotoxic Effect as Dual EGFR/VEGFR-2 Inhibitors

Al-Wahaibi, Lamya H.; Elshamsy, Ali M.; Ali, Taha F. S.; Youssif, Bahaa G. M.; Bräse, Stefan 1; Abdel-Aziz, Mohamed; El-Koussi, Nawal A.
1 Institut für Biologische und Chemische Systeme (IBCS), Karlsruher Institut für Technologie (KIT)

Abstract:

We developed and synthesized tetrahydropyrimidine derivatives as possible cytotoxic agents to inhibit EGFR and VEGFR-2 in the present study. Our study completely assesses the cytotoxic efficiency of pyrimidine-based derivatives 4–15 against various cancer cell lines, revealing derivatives 12 and 15 for their remarkable activity with GI50 values of 37 and 35 nM, respectively, when compared to the reference erlotinib (33 nM). In vitro enzyme assays showed that target compounds, particularly 12, 14, and 15, effectively inhibited EGFR and VEGFR-2. In vitro enzyme testing revealed that compound 15 was the most promising, with IC50 values of 84 and 3.50 nM for EGFR and VEGFR-2, respectively. Additionally, an in vitro assessment of the novel targets’ apoptotic potential revealed that both pro-apoptotic and antiapoptotic behaviors were promising, indicating that the apoptotic induction pathway is a strongly proposed action method for the newly developed targets. Finally, molecular docking experiments are elaborately discussed to corroborate the exact binding interactions of the most active hybrids 12 and 15 with the EGFR and VEGFR-2 active sites.


Verlagsausgabe §
DOI: 10.5445/IR/1000173562
Veröffentlicht am 27.08.2024
Originalveröffentlichung
DOI: 10.1021/acsomega.4c01361
Scopus
Zitationen: 7
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Zitationen: 7
Cover der Publikation
Zugehörige Institution(en) am KIT Institut für Biologische und Chemische Systeme (IBCS)
Publikationstyp Zeitschriftenaufsatz
Publikationsdatum 13.08.2024
Sprache Englisch
Identifikator ISSN: 2470-1343
KITopen-ID: 1000173562
Erschienen in ACS Omega
Verlag American Chemical Society (ACS)
Band 9
Heft 32
Seiten 34358–34369
Bemerkung zur Veröffentlichung Gefördert durch den KIT-Publikationsfonds
Vorab online veröffentlicht am 01.08.2024
Nachgewiesen in Web of Science
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Scopus
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