PADI3 通过靶向 CKS1 诱导的结肠癌信号转导抑制上皮-间质转化。

Zhengbin Chai, Changhui Zhu, Xiwei Wang, Yingying Zheng, Fabin Han, Qi Xie, Chunyan Liu
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引用次数: 0

摘要

背景:精氨酸脱氨酶 3(PADI3)参与人类疾病的各种生物学过程。最近,PADI3 因其在肿瘤发生中的作用而受到越来越多的关注。在之前的研究中,我们发现 PADI3 通过诱导细胞周期停滞在结肠癌中发挥抑瘤作用,但其在癌症转移中的关键作用和机制仍不清楚。本研究全面研究了 PADI3 在结肠癌细胞转移中的作用:Western印迹法检测相关蛋白的表达水平,Transwell法和伤口愈合法检测细胞迁移能力。流式细胞术用于测量和排除细胞凋亡对细胞迁移的影响。采用过表达和拯救实验来阐明 CKS1 在结肠癌细胞中的分子机制:结果:PADI3和CKS1的表达水平呈负相关,PADI3能以泛素依赖的方式促进CKS1的降解。PADI3可通过抑制CKS1的表达来抑制结肠癌细胞的迁移并降低伤口愈合速度。分子机制表明,CKS1可通过增加蜗牛和N-cadherin的表达、抑制E-cadherin的表达来促进EMT。PADI3作为CKS1的抑制因子,可以通过影响CKS1诱导的Snail上调和E-cadherin下调来阻断EMT的过程;但N-cadherin的表达却无法被挽救:结论:CKS1通过调节Snail/E-cadherin的表达促进结肠癌的EMT,而PADI3可以通过泛素依赖性方式促进CKS1降解来逆转这种效应。
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PADI3 inhibits epithelial-mesenchymal transition by targeting CKS1-induced signal transduction in colon cancer.

Background: Protein arginine deiminase 3 (PADI3) is involved in various biological processes of human disease. PADI3 has recently received increasing attention due to its role in tumorigenesis. In a previous study, we found that PADI3 plays a tumor suppressor role in colon cancer by inducing cell cycle arrest, but its critical role and mechanism in cancer metastasis remain obscure. In this study, we fully studied the role of PADI3 in colon cancer cell metastasis.

Methods: The expression levels of related proteins were detected by Western blotting, and Transwell and wound healing assays were used to examine the cell migration ability. Flow cytometry was used to measure and exclude cell apoptosis-affected cell migration. Both overexpression and rescue experiments were employed to elucidate the molecular mechanism of CKS1 in colon cancer cells.

Results: The expression levels of PADI3 and CKS1 are negatively related, and PADI3 can promote CKS1 degradation in a ubiquitin-dependent manner. PADI3 can suppress colon cancer cell migration and reduce the wound healing speed by inhibiting CKS1 expression. The molecular mechanism showed that CKS1 can promote EMT by increasing Snail and N-cadherin expression and suppressing E-cadherin expression. PADI3, as a suppressor of CKS1, can block the process of EMT by impairing CKS1-induced Snail upregulation and E-cadherin downregulation; however, the expression of N-cadherin cannot be rescued.

Conclusions: CKS1 promotes EMT in colon cancer by regulating Snail/E-cadherin expression, and this effect can be reversed by PADI3 via the promotion of CKS1 degradation in a ubiquitylation-dependent manner.

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