National Laboratory CIB (LNCIB), Area Science Park Padriciano, Trieste 34149, Italy.
Department of Life Sciences, University of Trieste, Trieste 34127, Italy.
Nat Commun. 2017 Jun 9;8:15772. doi: 10.1038/ncomms15772.
The prolyl isomerase PIN1, a critical modifier of multiple signalling pathways, is overexpressed in the majority of cancers and its activity strongly contributes to tumour initiation and progression. Inactivation of PIN1 function conversely curbs tumour growth and cancer stem cell expansion, restores chemosensitivity and blocks metastatic spread, thus providing the rationale for a therapeutic strategy based on PIN1 inhibition. Notwithstanding, potent PIN1 inhibitors are still missing from the arsenal of anti-cancer drugs. By a mechanism-based screening, we have identified a novel covalent PIN1 inhibitor, KPT-6566, able to selectively inhibit PIN1 and target it for degradation. We demonstrate that KPT-6566 covalently binds to the catalytic site of PIN1. This interaction results in the release of a quinone-mimicking drug that generates reactive oxygen species and DNA damage, inducing cell death specifically in cancer cells. Accordingly, KPT-6566 treatment impairs PIN1-dependent cancer phenotypes in vitro and growth of lung metastasis in vivo.
脯氨酰异构酶 PIN1 是多种信号通路的关键调节因子,在大多数癌症中过表达,其活性强烈促进肿瘤的发生和发展。相反,PIN1 功能的失活会抑制肿瘤生长和癌症干细胞扩增,恢复化疗敏感性并阻断转移扩散,从而为基于 PIN1 抑制的治疗策略提供了依据。然而,有效的 PIN1 抑制剂在抗癌药物中仍然缺乏。通过基于机制的筛选,我们已经鉴定出一种新型的共价 PIN1 抑制剂 KPT-6566,它能够选择性地抑制 PIN1 并将其靶向降解。我们证明 KPT-6566 与 PIN1 的催化位点发生共价结合。这种相互作用导致释放出一种类似醌的药物,产生活性氧和 DNA 损伤,特异性诱导癌细胞死亡。因此,KPT-6566 处理在体外损害了依赖 PIN1 的癌症表型,并在体内抑制了肺转移的生长。
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