The molecular mechanism underlying KRAS regulation on STK31 expression in pancreatic ductal adenocarcinoma

IF 4.5 2区 医学 Q1 ONCOLOGY Cancer Science Pub Date : 2024-07-25 DOI:10.1111/cas.16286
Yuting Liu, Shing Chun Tang, Chi Han Li, Ka Fai To, Bo Li, Stephen Lam Chan, Chi Hin Wong, Yangchao Chen
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Abstract

KRAS gene mutations are common in pancreatic ductal adenocarcinoma (PDAC), but targeting mutant KRAS is still challenging. Here, an endoribonuclease-prepared small interfering RNA (esiRNA) library was used to screen new kinases that play critical roles in PDAC driven by KRAS gene mutations, and serine/threonine kinase 31 (STK31) was identified and characterized as a potential therapeutic target for KRAS-mutant PDAC. Our results showed that STK31 was upregulated in KRAS-mutant PDAC patients with poor survival and highly expressed in PDAC cell lines with KRASG12D mutation. Inhibition of STK31 in KRAS-mutant cell lines significantly reduced PDAC cell growth in vitro and hindered tumor growth in vivo. Gain and loss of function experiments revealed that STK31 is a downstream target of KRAS in PDAC. A pharmacological inhibition assay showed MAPK/ERK signaling involved in STK31 regulation. The further mechanistic study validated that c-Jun, regulated by KRAS/MAPK signaling, directly modulates the transcription level of STK31 by binding to its promoter region. Through RNA sequencing, we found that the cell cycle regulators CCNB1 and CDC25C are downstream targets of STK31. Taken together, our results indicate that STK31, which is the downstream target of the KRAS/MAPK/ERK/c-Jun signaling pathway in KRAS-mutant PDAC, promotes PDAC cell growth by modulating the expression of the cell cycle regulators CCNB1 and CDC25C.

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胰腺导管腺癌中 KRAS 调控 STK31 表达的分子机制。
KRAS 基因突变在胰腺导管腺癌(PDAC)中很常见,但靶向突变的 KRAS 仍具有挑战性。在这里,我们利用内切核酸酶制备的小干扰RNA(esiRNA)文库筛选了在KRAS基因突变驱动的PDAC中发挥关键作用的新激酶,并确定丝氨酸/苏氨酸激酶31(STK31)为KRAS突变PDAC的潜在治疗靶点。我们的研究结果表明,STK31在KRAS突变的PDAC患者中上调,而这些患者的生存率很低,STK31在KRASG12D突变的PDAC细胞系中高表达。抑制 KRAS 突变细胞株中的 STK31 能显著降低 PDAC 细胞在体外的生长,并阻碍肿瘤在体内的生长。功能增益和缺失实验显示,STK31 是 KRAS 在 PDAC 中的下游靶点。药理抑制实验表明,MAPK/ERK 信号转导参与了 STK31 的调控。进一步的机理研究验证了受 KRAS/MAPK 信号调控的 c-Jun 通过与其启动子区域结合直接调节 STK31 的转录水平。通过 RNA 测序,我们发现细胞周期调控因子 CCNB1 和 CDC25C 是 STK31 的下游靶标。综上所述,我们的研究结果表明,STK31是KRAS/MAPK/ERK/c-Jun信号通路在KRAS突变型PDAC中的下游靶点,它通过调节细胞周期调节因子CCNB1和CDC25C的表达来促进PDAC细胞的生长。
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来源期刊
Cancer Science
Cancer Science 医学-肿瘤学
自引率
3.50%
发文量
406
审稿时长
2 months
期刊介绍: Cancer Science (formerly Japanese Journal of Cancer Research) is a monthly publication of the Japanese Cancer Association. First published in 1907, the Journal continues to publish original articles, editorials, and letters to the editor, describing original research in the fields of basic, translational and clinical cancer research. The Journal also accepts reports and case reports. Cancer Science aims to present highly significant and timely findings that have a significant clinical impact on oncologists or that may alter the disease concept of a tumor. The Journal will not publish case reports that describe a rare tumor or condition without new findings to be added to previous reports; combination of different tumors without new suggestive findings for oncological research; remarkable effect of already known treatments without suggestive data to explain the exceptional result. Review articles may also be published.
期刊最新文献
Issue Information In this issue Issue Information In this issue Real-world genome profiling in Japanese patients with pancreatic ductal adenocarcinoma focusing on HRD implications
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