Pin1 抑制作用能有效抑制胃癌生长,并阻断 PI3K/AKT 和 Wnt/β-catenin 致癌通路。
Pin1 inhibition potently suppresses gastric cancer growth and blocks PI3K/AKT and Wnt/β-catenin oncogenic pathways.
机构信息
Fujian Key Laboratory for Translational Research in Cancer and Neurodegenerative Diseases, Institute for Translational Medicine, Fujian Medical University, Fuzhou, Fujian, China.
Department of Pathology, The First Affiliated Hospital of Fujian Medical University, Fuzhou, Fujian, China.
出版信息
Mol Carcinog. 2019 Aug;58(8):1450-1464. doi: 10.1002/mc.23027. Epub 2019 Apr 26.
Gastric cancer is the second leading cause of cancer-related mortality and the fourth most common cancer globally. High intratumor heterogeneity of advanced gastric cancer poses great challenges to targeted therapy due to simultaneous activation of many redundant cancer-driving pathways. A central common signaling mechanism in cancer is proline-directed phosphorylation, which is further regulated by the unique proline isomerase Pin1. Pin1 inhibition exerts anticancer activity by blocking multiple cancer-driving pathways in some cancers, but its role in gastric cancer is not fully understood. Here we detected Pin1 protein expression in 1065 gastric cancer patients and paired normal tissues using immunohistochemistry and Western blot, and then examined the effects of Pin1 overexpression, and genetic and chemical Pin1 inhibition using Pin1 short hairpin RNA or small molecule inhibitor all-trans retinoic acid (ATRA) on tumorigenesis of human gastric cancer in vitro and in vivo, followed by biochemical analyses to elucidate Pin1 regulated oncogenic pathways. We found that Pin1 was significantly overexpressed in primary and metastasized tumors, with Pin1 overexpression being correlated with advanced stage and poor prognosis. Furthermore, whereas Pin1 overexpression promoted the transformed phenotype in immortalized and nontransformed human gastric cells, either genetic or chemical Pin1 inhibition in multiple human gastric cancer cells potently suppressed cell growth, G1/S transition and colony formation in vitro, as well as tumor growth in xenograft tumor models in vivo, which were further supported by downregulation of multiple key oncoproteins in PI3K/AKT and Wnt/β-catenin signaling pathways. These results not only provide the first evidence for a critical role of Pin1 in the tumorigenesis of gastric cancer but also suggest that targeting Pin1 using ATRA or other inhibitors offers an effective new therapeutic approach for treating advanced gastric cancer.
胃癌是癌症相关死亡的第二大主要原因,也是全球第四大最常见的癌症。由于许多冗余的致癌途径同时被激活,晚期胃癌的肿瘤内异质性很高,这给靶向治疗带来了巨大的挑战。癌症中的一个核心共同信号机制是脯氨酸定向磷酸化,它进一步受到独特的脯氨酸异构酶 Pin1 的调节。Pin1 抑制通过阻断一些癌症中的多个致癌途径发挥抗癌活性,但它在胃癌中的作用尚未完全阐明。在这里,我们使用免疫组织化学和 Western blot 检测了 1065 例胃癌患者和配对正常组织中的 Pin1 蛋白表达,然后检查了 Pin1 过表达以及遗传和化学 Pin1 抑制(使用 Pin1 短发夹 RNA 或小分子抑制剂全反式视黄酸(ATRA))对体外和体内人胃癌肿瘤发生的影响,然后进行生化分析以阐明 Pin1 调节的致癌途径。我们发现,Pin1 在原发性和转移性肿瘤中均明显过表达,Pin1 过表达与晚期和预后不良相关。此外,虽然 Pin1 过表达促进了永生化和未转化的人胃细胞的转化表型,但在多种人胃癌细胞中,遗传或化学 Pin1 抑制均可强力抑制细胞生长、G1/S 过渡和体外集落形成,以及体内异种移植肿瘤模型中的肿瘤生长,这进一步得到了 PI3K/AKT 和 Wnt/β-catenin 信号通路中多个关键癌蛋白下调的支持。这些结果不仅为 Pin1 在胃癌发生中的关键作用提供了首个证据,还表明使用 ATRA 或其他抑制剂靶向 Pin1 为治疗晚期胃癌提供了一种有效的新治疗方法。
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