(Thio)chromenone derivatives exhibit anti-metastatic effects through selective inhibition of uPAR in cancer cell lines: discovery of an uPAR-targeting fluorescent probe

(Thio)chromenone derivatives exhibit anti-metastatic effects through selective inhibition of uPAR in cancer cell lines: discovery of an uPAR-targeting fluorescent probe

A class of (thio)chromenone derivatives has been identified as suitable ligands for uPAR, a glycoprotein with a prognostic value in a large number of human cancers. The (thio)chromenone agents actively inhibited the binding of uPAR to uPA with a binding affinity of 18.6 nM, reducing cell migration i...

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Veröffentlicht in:Chemical communications (Cambridge, England) England), 2025-01, Vol.61 (5), p.909-912
Hauptverfasser: Chun, So-Young, Park, Chanhee, Oh, Jiwon, Yoon, Hey-Jin, Kim, Tae-Il, Kim, Youngmi, Ham, Seung Wook, Koh, Hye Ran, Lee, Hyung Ho, Kim, Hun Young, Oh, Kyungsoo
Format: Artikel
Sprache:eng
Schlagworte:
Antineoplastic Agents - chemical synthesis
Antineoplastic Agents - chemistry
Antineoplastic Agents - pharmacology
Benzopyrans - chemical synthesis
Benzopyrans - chemistry
Benzopyrans - pharmacology
Binding
Cancer
Cell Line, Tumor
Cell Movement - drug effects
Drug Screening Assays, Antitumor
Fluorescent Dyes - chemical synthesis
Fluorescent Dyes - chemistry
Fluorescent Dyes - pharmacology
Fluorescent indicators
Glycoproteins
Humans
Molecular Structure
Receptors, Urokinase Plasminogen Activator - antagonists & inhibitors
Receptors, Urokinase Plasminogen Activator - metabolism
Wound healing
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Beschreibung
Zusammenfassung:A class of (thio)chromenone derivatives has been identified as suitable ligands for uPAR, a glycoprotein with a prognostic value in a large number of human cancers. The (thio)chromenone agents actively inhibited the binding of uPAR to uPA with a binding affinity of 18.6 nM, reducing cell migration in the wound healing assay by up to 40% without apparent cell motility. The discovery of an uPAR-targeting fluorescent probe was also made in this study that can selectively bind to the membrane uPAR, providing valuable molecular insights into the role of uPAR in cancer metastasis. This study should serve as a basis for the development of new uPAR-targeting agents that can control the metastatic potential of cancer cells with minimal cytotoxicity.
ISSN:1359-7345
1364-548X
1364-548X
DOI:10.1039/d4cc05907g