Hsa_circ_0007590/PTBP1 complex reprograms glucose metabolism by reducing the stability of m6A-modified PTEN mRNA in pancreatic ductal adenocarcinoma

IF 4.8 3区 医学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Dandan Zheng, Wenying Chen, Juanfei Peng, Xianxian Huang, Shineng Zhang, Yanyan Zhuang
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Abstract

The role of circular RNAs (circRNAs) in glucose metabolism in pancreatic duct adenocarcinoma (PDAC) remains elusive. Through RNA sequencing of cells cultured under conditions of glucose deprivation, we identified hsa_circ_0007590. Sanger sequencing and RNase R and Act D treatments were performed to confirm the circular RNA features of hsa_circ_0007590. RNA in situ hybridization (RNA-ISH) and quantitative reverse transcription PCR (qRT-PCR) were used to estimate hsa_circ_0007590 expression in PDAC clinical specimens and cell lines. hsa_circ_0007590 expression was higher in PDAC patients and closely related to the clinicopathological characteristics of the disease. Cytoplasm‒nuclear fractionation and FISH assays demonstrated that hsa_circ_0007590 was located in the nucleus. Gain-of-function and loss-of-function assays were performed to assess the biological behaviors of PDAC cells. Seahorse XF assays were performed to validate the Warburg effect. hsa_circ_0007590 facilitated the proliferation, migration, and invasion of PDAC cells and promoted the Warburg effect. Mass spectrometry, RNA pulldown, RNA immunoprecipitation (RIP), RNA m6A quantification, m6A dot blot, MeRIP, and Western blotting were conducted to investigate the detailed mechanism through which hsa_circ_0007590 produces these effects. Mechanistically, hsa_circ_0007590 targeted PTBP1 and increased the expression of the m6A reader protein YTHDF2, leading to PTEN mRNA degradation and PI3K/AKT/mTOR pathway activation. Overall, hsa_circ_0007590, which targets PTBP1, reprograms glucose metabolism by attenuating the stability of m6A-modified PTEN mRNA and holds potential promise as a therapeutic target for PDAC.

Abstract Image

Abstract Image

Hsa_circ_0007590/PTBP1 复合物通过降低胰腺导管腺癌中 m6A 修饰的 PTEN mRNA 的稳定性来重编葡萄糖代谢。
环状 RNA(circRNA)在胰管腺癌(PDAC)葡萄糖代谢中的作用仍然难以捉摸。通过对葡萄糖剥夺条件下培养的细胞进行 RNA 测序,我们发现了 hsa_circ_0007590。为了确认 hsa_circ_0007590 的环状 RNA 特征,我们进行了 Sanger 测序以及 RNase R 和 Act D 处理。采用 RNA 原位杂交(RNA-ISH)和定量反转录 PCR(qRT-PCR)估测了 hsa_circ_0007590 在 PDAC 临床标本和细胞系中的表达情况,发现 hsa_circ_0007590 在 PDAC 患者中的表达较高,且与疾病的临床病理特征密切相关。细胞质-核分馏和 FISH 检测表明,hsa_circ_0007590 位于细胞核中。为了评估 PDAC 细胞的生物学行为,进行了功能增益和功能缺失试验。hsa_circ_0007590 促进了 PDAC 细胞的增殖、迁移和侵袭,并促进了沃伯格效应。质谱分析、RNA pulldown、RNA免疫沉淀(RIP)、RNA m6A定量、m6A点印迹、MeRIP和Western印迹研究了hsa_circ_0007590产生这些效应的详细机制。从机制上讲,hsa_circ_0007590 以 PTBP1 为靶标,增加了 m6A 阅读蛋白 YTHDF2 的表达,导致 PTEN mRNA 降解和 PI3K/AKT/mTOR 通路激活。总之,hsa_circ_0007590以PTBP1为靶点,通过降低m6A修饰的PTEN mRNA的稳定性来重新规划葡萄糖代谢,有望成为PDAC的治疗靶点。
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来源期刊
Cancer gene therapy
Cancer gene therapy 医学-生物工程与应用微生物
CiteScore
10.20
自引率
0.00%
发文量
150
审稿时长
4-8 weeks
期刊介绍: Cancer Gene Therapy is the essential gene and cellular therapy resource for cancer researchers and clinicians, keeping readers up to date with the latest developments in gene and cellular therapies for cancer. The journal publishes original laboratory and clinical research papers, case reports and review articles. Publication topics include RNAi approaches, drug resistance, hematopoietic progenitor cell gene transfer, cancer stem cells, cellular therapies, homologous recombination, ribozyme technology, antisense technology, tumor immunotherapy and tumor suppressors, translational research, cancer therapy, gene delivery systems (viral and non-viral), anti-gene therapy (antisense, siRNA & ribozymes), apoptosis; mechanisms and therapies, vaccine development, immunology and immunotherapy, DNA synthesis and repair. Cancer Gene Therapy publishes the results of laboratory investigations, preclinical studies, and clinical trials in the field of gene transfer/gene therapy and cellular therapies as applied to cancer research. Types of articles published include original research articles; case reports; brief communications; review articles in the main fields of drug resistance/sensitivity, gene therapy, cellular therapy, tumor suppressor and anti-oncogene therapy, cytokine/tumor immunotherapy, etc.; industry perspectives; and letters to the editor.
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