Regulation of a novel circATP8B4/miR-31-5p/nestin ceRNA crosstalk in proliferation, motility, invasion and radiosensitivity of human glioma cells

IF 1.9 4区 医学 Q2 BIOLOGY Journal of Radiation Research Pub Date : 2024-09-17 DOI:10.1093/jrr/rrae064
Dongdong Luo, Aiping Luo, Ganwei Ye, Dan Li, Su Hu, Hailin Zhao, Biao Peng
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Abstract

Deregulation of circular RNAs (circRNAs) is frequent in human glioma. Although circRNA ATPase phospholipid transporting 8B4 (circATP8B4) is highly expressed in glioma, its precise action in glioma development is still not fully understood. The relationship of microRNA (miR)-31-5p and circATP8B4 or nestin (NES) was predicted by bioinformatic analysis and confirmed by RNA pull-down and Dual-luciferase reporter assays. CircATP8B4, miR-31-5p and NES were quantified by qRT-PCR or western blot. Cell functional behaviors were assessed by EdU, wound-healing and transwell invasion assays. Xenograft model experiments were performed to define circATP8B4’s activity in vivo. CircATP8B4, a true circular transcript, was upregulated in human glioma. CircATP8B4 downregulation weakened glioma cell growth, motility, and invasion and facilitated radiosensitivity. Mechanistically, circATP8B4 and NES 3′UTR harbored a shared miR-31-5p pairing site, and circATP8B4 involved the post-transcriptional NES regulation by functioning as a competing endogenous RNA (ceRNA). Furthermore, the miR-31-5p/NES axis participated in circATP8B4’s activity in glioma cell proliferation, motility, invasion and radiosensitivity. Additionally, circATP8B4 loss diminished tumor growth and enhanced the anticancer effect of radiotherapy in vivo. We have uncovered an uncharacterized ceRNA cascade, circATP8B4/miR-31-5p/NES axis, underlying glioma development and radiosensitivity. Targeting the ceRNA crosstalk may have potential to improve the outcome of glioma patients.
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新型 circATP8B4/miR-31-5p/nestin ceRNA 在人类胶质瘤细胞增殖、运动、侵袭和放射敏感性中的串联调控作用
人类胶质瘤中经常出现环状 RNA(circRNA)的失调。虽然循环RNA ATP酶磷脂转运8B4(circATP8B4)在胶质瘤中高表达,但其在胶质瘤发展过程中的确切作用仍未完全明了。通过生物信息学分析预测了microRNA(miR)-31-5p与circATP8B4或nestin(NES)的关系,并通过RNA牵引和双荧光素酶报告实验证实了这种关系。通过 qRT-PCR 或 Western 印迹对 CircATP8B4、miR-31-5p 和 NES 进行了定量。细胞功能行为通过 EdU、伤口愈合和跨孔侵袭实验进行评估。为了确定 circATP8B4 在体内的活性,还进行了异种移植模型实验。CircATP8B4 是一种真正的环形转录本,在人类胶质瘤中上调。下调 CircATP8B4 会削弱胶质瘤细胞的生长、运动和侵袭能力,并提高放射敏感性。从机制上看,circATP8B4和NES 3′UTR含有一个共享的miR-31-5p配对位点,circATP8B4通过作为竞争性内源性RNA(ceRNA)参与转录后NES调控。此外,miR-31-5p/NES 轴参与了 circATP8B4 在胶质瘤细胞增殖、运动、侵袭和放射敏感性方面的活性。此外,circATP8B4 的缺失会减少肿瘤的生长,并增强体内放疗的抗癌效果。我们发现了一种尚未定性的ceRNA级联,即circATP8B4/miR-31-5p/NES轴,它是胶质瘤发展和放射敏感性的基础。以 ceRNA 串联为靶点可能会改善胶质瘤患者的预后。
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来源期刊
CiteScore
3.60
自引率
5.00%
发文量
86
审稿时长
4-8 weeks
期刊介绍: The Journal of Radiation Research (JRR) is an official journal of The Japanese Radiation Research Society (JRRS), and the Japanese Society for Radiation Oncology (JASTRO). Since its launch in 1960 as the official journal of the JRRS, the journal has published scientific articles in radiation science in biology, chemistry, physics, epidemiology, and environmental sciences. JRR broadened its scope to include oncology in 2009, when JASTRO partnered with the JRRS to publish the journal. Articles considered fall into two broad categories: Oncology & Medicine - including all aspects of research with patients that impacts on the treatment of cancer using radiation. Papers which cover related radiation therapies, radiation dosimetry, and those describing the basis for treatment methods including techniques, are also welcomed. Clinical case reports are not acceptable. Radiation Research - basic science studies of radiation effects on livings in the area of physics, chemistry, biology, epidemiology and environmental sciences. Please be advised that JRR does not accept any papers of pure physics or chemistry. The journal is bimonthly, and is edited and published by the JRR Editorial Committee.
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