Isoleucyl-tRNA synthetase 2 promotes pancreatic ductal adenocarcinoma proliferation and metastasis by stabilizing β-catenin

IF 6.9 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Genes & Diseases Pub Date : 2024-07-24 DOI:10.1016/j.gendis.2024.101382
Yixun Jin, Xinyang Huang, Zhuoxin Wang, Berik Kouken, Qi Wang, Lifu Wang
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Abstract

Isoleucyl-tRNA synthetase 2 (IARS2), originally regarded as an enzyme ligating isoleucine to the corresponding tRNA, has been identified as an oncogene recently. However, its function in pancreatic ductal adenocarcinoma (PDAC) remains to be discovered. Here we explored the biological role of IARS2 in PDAC. Up-regulated IARS2 was found in PDAC tissues and cell lines. Kaplan-Meier survival analysis indicated a worse prognosis in patients with high IARS2 expression. CCK-8, EdU, and colony formation assays showed IARS2 overexpression enhanced PDAC proliferation, which was reduced by IARS2 knockdown. Meanwhile, IARS2 down-regulation inhibited PDAC metastasis by impeding epithelial–mesenchymal transition. These results were also supported by subcutaneous xenograft and metastasis assays . To figure out underlying mechanisms, differential and enrichment analyses were conducted and the WNT signaling pathway was discovered. Our results demonstrated that there was no significant relationship between the WNT signaling pathway key factor CTNNB1 and IARS2 at the transcription level. However, cycloheximide assays showed that IARS2 reduced the β-catenin degradation rate. IARS2 inhibited the phosphorylation of β-catenin at the Ser33/37 site and regulated downstream targets of WNT signaling including c-MYC, c-JUN, and MMP7. The enhancement of proliferation and metastasis caused by IARS2 could be reversed by MSAB, an agent that promotes β-catenin degradation. In summary, IARS2 facilitates PDAC proliferation and metastasis by stabilizing β-catenin, which leads to WNT/β-catenin activation. IARS2 serves as an underlying prognosis marker and a potential therapeutic target for PDAC.
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异亮氨酰-tRNA合成酶2通过稳定β-catenin促进胰腺导管腺癌的增殖和转移
异亮氨酰-tRNA合成酶2(IARS2)最初被认为是一种将异亮氨酸连接到相应tRNA的酶,最近被确定为一种癌基因。然而,它在胰腺导管腺癌(PDAC)中的功能仍有待发现。在此,我们探讨了 IARS2 在 PDAC 中的生物学作用。在 PDAC 组织和细胞系中发现了上调的 IARS2。Kaplan-Meier生存分析表明,IARS2高表达的患者预后较差。CCK-8、EdU和集落形成试验表明,IARS2过表达会增强PDAC的增殖,而IARS2基因敲除会减少增殖。同时,IARS2 的下调通过阻碍上皮-间质转化抑制了 PDAC 的转移。皮下异种移植和转移实验也证实了这些结果。为了找出潜在的机制,我们进行了差异和富集分析,并发现了 WNT 信号通路。我们的结果表明,WNT 信号通路关键因子 CTNNB1 与 IARS2 在转录水平上没有显著关系。然而,环己亚胺试验表明,IARS2降低了β-catenin的降解率。IARS2抑制了β-catenin在Ser33/37位点的磷酸化,并调控了WNT信号转导的下游靶标,包括c-MYC、c-JUN和MMP7。促进β-catenin降解的药物MSAB可逆转IARS2对增殖和转移的促进作用。总之,IARS2通过稳定β-catenin促进PDAC的增殖和转移,从而导致WNT/β-catenin活化。IARS2是潜在的预后标志物,也是PDAC的潜在治疗靶点。
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来源期刊
Genes & Diseases
Genes & Diseases Multiple-
CiteScore
7.30
自引率
0.00%
发文量
347
审稿时长
49 days
期刊介绍: Genes & Diseases is an international journal for molecular and translational medicine. The journal primarily focuses on publishing investigations on the molecular bases and experimental therapeutics of human diseases. Publication formats include full length research article, review article, short communication, correspondence, perspectives, commentary, views on news, and research watch. Aims and Scopes Genes & Diseases publishes rigorously peer-reviewed and high quality original articles and authoritative reviews that focus on the molecular bases of human diseases. Emphasis will be placed on hypothesis-driven, mechanistic studies relevant to pathogenesis and/or experimental therapeutics of human diseases. The journal has worldwide authorship, and a broad scope in basic and translational biomedical research of molecular biology, molecular genetics, and cell biology, including but not limited to cell proliferation and apoptosis, signal transduction, stem cell biology, developmental biology, gene regulation and epigenetics, cancer biology, immunity and infection, neuroscience, disease-specific animal models, gene and cell-based therapies, and regenerative medicine.
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