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Antitumor effects of new glycoconjugated Pt agents dual-targeting GLUT1 and Pgp proteins

Dalton Transactions, ISSN: 1477-9234, Vol: 51, Issue: 42, Page: 16082-16092
2022
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Article Description

A novel and highly efficient dual-targeting Pt system was designed to improve the drug delivery capacity and selectivity in cancer treatment. The dual-targeting monofunctional Pt complexes (1-8) having glycosylated pendants as tridentated ligand were achieved by introducing glycosylation modification in the thioaminocarbazone compounds with potential lysosomal targeting ability. The structures and stability of 1-8 were further established by various techniques. Molecular docking studies showed that 2 was efficiently docked into glucose transporters protein 1 (GLUT1) and P-glycoprotein (Pgp) proteins with the optimal CDocker-interaction-energy of −64.84 and −48.85 kcal mol. Complex 2 with higher protein binding capacity demonstrated significant and broad-spectrum antitumor efficacy in vitro, even exhibiting a half maximal inhibitory concentration (IC) value (∼10 μM) than cisplatin (∼17 μM) against human lung adenocarcinoma cells (A549). The inhibitor experiment revealed GLUT-mediated uptake of 2, and the subcellular localization experiment in A549 also proved that 2 could be localized in the lysosome, thereby causing cell apoptosis. Moreover, cellular thermal shift assay (CETSA) confirmed the binding of 2 with the target proteins of GLUT1 and Pgp. The above results indicated that 2 represents a potential anticancer candidate with dual-targeting functions.

Bibliographic Details

Zhang, Qiang; Shao, Jia; Wang, Jin; Gong, Xian-Jin; Liu, Wei-Xing; Wang, Shan; Zhang, Yi; Yang, Shuang; Zhang, Quan-Sheng; Wei, Jin-Xia; Tian, Jin-Lei

Royal Society of Chemistry (RSC)

Chemistry

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