（Thio）染色体衍生物通过选择性抑制癌细胞系中的uPAR表现出抗转移作用：发现一种靶向uPAR的荧光探针。

IF 4.2 2区化学 Q2 CHEMISTRY, MULTIDISCIPLINARY

Chemical Communications Pub Date : 2024-11-22 DOI:10.1039/d4cc05907g

So-Young Chun , Chanhee Park , Jiwon Oh , Hey-Jin Yoon , Tae-il Kim , Youngmi Kim , Seung Wook Ham , Hye Ran Koh , Hyung Ho Lee , Hun Young Kim , Kyungsoo Oh

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引用次数: 0

摘要

一类（硫）染色体衍生物已被确定为uPAR的合适配体，uPAR是一种在许多人类癌症中具有预后价值的糖蛋白。（硫）铬酮药物以18.6 nM的结合亲和力积极抑制uPAR与uPA的结合，在伤口愈合实验中减少了高达40%的细胞迁移，而没有明显的细胞运动性。本研究还发现了一种靶向uPAR的荧光探针，可以选择性地结合膜uPAR，为uPAR在癌症转移中的作用提供了有价值的分子见解。这项研究应该为开发新的upar靶向药物奠定基础，这些药物可以以最小的细胞毒性控制癌细胞的转移潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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

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(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 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.

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来源期刊

Chemical Communications 化学-化学综合

CiteScore

8.60

自引率

4.10%

发文量

2705

审稿时长

1.4 months

期刊介绍： ChemComm (Chemical Communications) is renowned as the fastest publisher of articles providing information on new avenues of research, drawn from all the world''s major areas of chemical research.