SFPQ promotes RAS-mutant cancer cell growth by modulating 5'-UTR mediated translational control of CK1α.

NAR Cancer Pub Date : 2022-09-27 eCollection Date: 2022-09-01 DOI:10.1093/narcan/zcac027
Venetia Jing Tong Kok, Jia Ying Tang, Gracie Wee Ling Eng, Shin Yi Tan, Joseph Tin Foong Chin, Chun Hian Quek, Wei Xuan Lai, Teck Kwang Lim, Qingsong Lin, John Jia En Chua, Jit Kong Cheong
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Abstract

Oncogenic mutations in the RAS family of small GTPases are commonly found in human cancers and they promote tumorigenesis by altering gene expression networks. We previously demonstrated that Casein Kinase 1α (CK1α), a member of the CK1 family of serine/threonine kinases, is post-transcriptionally upregulated by oncogenic RAS signaling. Here, we report that the CK1α mRNA contains an exceptionally long 5'-untranslated region (UTR) harbouring several translational control elements, implicating its involvement in translational regulation. We demonstrate that the CK1α 5'-UTR functions as an IRES element in HCT-116 colon cancer cells to promote cap-independent translation. Using tobramycin-affinity RNA-pulldown assays coupled with identification via mass spectrometry, we identified several CK1α 5'-UTR-binding proteins, including SFPQ. We show that RNA interference targeting SFPQ reduced CK1α protein abundance and partially blocked RAS-mutant colon cancer cell growth. Importantly, transcript and protein levels of SFPQ and other CK1α 5'-UTR-associated RNA-binding proteins (RBPs) are found to be elevated in early stages of RAS-mutant cancers, including colorectal and lung adenocarcinoma. Taken together, our study uncovers a previously unappreciated role of RBPs in promoting RAS-mutant cancer cell growth and their potential to serve as promising biomarkers as well as tractable therapeutic targets in cancers driven by oncogenic RAS.

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SFPQ 通过调节 5'-UTR 介导的 CK1α 翻译控制,促进 RAS 突变癌细胞的生长。
小 GTP 酶 RAS 家族的致癌突变常见于人类癌症,它们通过改变基因表达网络促进肿瘤发生。我们以前曾证实,酪蛋白激酶 1α(CK1α)是丝氨酸/苏氨酸激酶 CK1 家族的成员之一,会因致癌 RAS 信号转导而转录后上调。在这里,我们报告了 CK1α mRNA 含有一个特别长的 5'- 非翻译区 (UTR),该区域含有多个翻译控制元件,这意味着它参与了翻译调控。我们证明,在 HCT-116 结肠癌细胞中,CK1α 5'-UTR 发挥着 IRES 元件的作用,以促进不依赖于帽子的翻译。通过妥布霉素亲和 RNA 推移试验以及质谱鉴定,我们发现了几种 CK1α 5'-UTR 结合蛋白,包括 SFPQ。我们发现,以 SFPQ 为靶点的 RNA 干扰降低了 CK1α 蛋白丰度,并部分阻断了 RAS 突变结肠癌细胞的生长。重要的是,在 RAS 突变癌症(包括结直肠癌和肺腺癌)的早期阶段,SFPQ 和其他 CK1α 5'-UTR 相关 RNA 结合蛋白(RBPs)的转录本和蛋白水平都会升高。综上所述,我们的研究揭示了 RBPs 在促进 RAS 突变癌细胞生长方面以前未被认识到的作用,以及它们在致癌 RAS 驱动的癌症中作为有前景的生物标志物和可治疗靶点的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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