Rab8 GTPase 通过直接调节其在人非小细胞肺癌中的表面表达来调节 Klotho 介导的细胞生长和进展抑制。
Rab8 GTPase regulates Klotho-mediated inhibition of cell growth and progression by directly modulating its surface expression in human non-small cell lung cancer.
机构信息
Jiangsu Provincial Key Laboratory of Geriatrics, Department of Geriatrics, Jiangsu Province Hospital, the First Affiliated Hospital of Nanjing Medical University, 300 Guangzhou Road, Nanjing, Jiangsu 210029, China; Johns Hopkins Institute for NanoBioTechnology, Johns Hopkins University, Baltimore, Maryland 21218, United States.
Institute of Basic Medicine, Shandong Academy of Medical Sciences, Jinan, Shandong 250000, China.
出版信息
EBioMedicine. 2019 Nov;49:118-132. doi: 10.1016/j.ebiom.2019.10.040. Epub 2019 Nov 6.
BACKGROUND
The klotho (KL) gene is an anti-aging gene that has recently been shown to also function as a general tumor suppressor. However, there is currently only limited information regarding the potential molecular signals for regulation of Klotho without identifying precise molecular mechanisms or interactions.
METHODS
We performed a mass spectrometry (MS) assay to screen candidate proteins complexed with Klotho derived from immunoprecipitation in human non-small cell lung cancer (NSCLC) cells, and identified Rab8 to be the protein that most prominently interacts with Klotho. We further investigated whether Rab8 can regulate trafficking of Klotho and which process it would modulate using surface biotinylation assay, immunofluorescence and fluorescence ratio microscopy. Furthermore, we explored whether Rab8 is involved in Klotho-mediated function in NSCLC, and verified the results which we found in vivo using xenograft mouse model.
FINDINGS
We report discovery of Rab8 as a Klotho-interacting protein that acts as a critical modulator of Klotho surface expression in human NSCLC. In particular, we report that Rab8 is co-localized and associated with Klotho, and Klotho trafficking is regulated by Rab8. Moreover, we found that Rab8 modulates surface levels of Klotho via a post-biosynthetic pathway, as opposed to an endocytic pathway. Furthermore, we demonstrate that Rab8 is involved in Klotho-mediated regulation of cell proliferation, migration, invasiveness, epithelial-mesenchymal transition (EMT), and Wnt-β-catenin signaling in NSCLC. Additionally, Rab8 overexpression was also found to increase Klotho-mediated inhibition of NSCLC tumorigenesis in vivo.
INTERPRETATION
Overall, our findings suggest that Rab8 GTPase can regulate Klotho-mediated inhibition of Wnt signaling activity by modulating translocation of Klotho onto the cell surface, which in turn affects Klotho-mediated inhibition of cell proliferation, migration and invasiveness in NSCLC. These results have important implications for the development of new therapeutic targets, Klotho-related research in the context of NSCLC as well as other areas, and provide a working model for Rab8 function in the context of cancer and cancer biology.
背景
klotho(KL)基因是一种抗衰老基因,最近已被证明也具有一般的肿瘤抑制作用。然而,目前关于 Klotho 的潜在分子信号调节的信息有限,而没有确定精确的分子机制或相互作用。
方法
我们进行了质谱(MS)测定,以筛选从人非小细胞肺癌(NSCLC)细胞的免疫沉淀中衍生的与 Klotho 复合的候选蛋白,并确定 Rab8 是与 Klotho 相互作用最显著的蛋白质。我们进一步研究了 Rab8 是否可以调节 Klotho 的运输,以及使用表面生物素化测定法、免疫荧光和荧光比显微镜来调节哪个过程。此外,我们探讨了 Rab8 是否参与 Klotho 在 NSCLC 中的介导功能,并通过异种移植小鼠模型验证了我们体内发现的结果。
结果
我们报告了 Rab8 作为 Klotho 相互作用蛋白的发现,它在人 NSCLC 中作为 Klotho 表面表达的关键调节剂。具体而言,我们报告 Rab8 与 Klotho 共定位和相关,并且 Klotho 的运输受到 Rab8 的调节。此外,我们发现 Rab8 通过翻译后途径而不是内吞途径调节 Klotho 的表面水平。此外,我们证明 Rab8 参与 Klotho 介导的 NSCLC 中细胞增殖、迁移、侵袭、上皮-间充质转化(EMT)和 Wnt-β-catenin 信号转导的调节。此外,还发现 Rab8 过表达也增加了体内 Klotho 介导的 NSCLC 肿瘤抑制作用。
解释
总体而言,我们的发现表明 Rab8 GTPase 可以通过调节 Klotho 向细胞表面的易位来调节 Klotho 介导的 Wnt 信号活性的抑制,从而影响 Klotho 介导的 NSCLC 中细胞增殖、迁移和侵袭的抑制。这些结果对开发新的治疗靶点、Klotho 在 NSCLC 以及其他领域的相关研究具有重要意义,并为 Rab8 在癌症和癌症生物学中的功能提供了工作模型。
Zotero 插件