在肝细胞癌中,LncRNA SNHG1通过吸收miR-199a-5p/3p上调FANCD2和G6PD以抑制脱铁性贫血。

IF 1.9 Q3 PHARMACOLOGY & PHARMACY Drug Discoveries and Therapeutics Pub Date : 2023-09-15 Epub Date: 2023-08-19 DOI:10.5582/ddt.2023.01035
Lin Zhou, Qing Zhang, Jiaxin Cheng, Xiandie Shen, Jing Li, Mingya Chen, Chang Zhou, Jianlin Zhou
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引用次数: 1

摘要

脱铁症是一种由铁依赖性脂质过氧化引发的调节性细胞死亡(RCD),与肝细胞癌(HCC)的发生和发展密切相关。lncRNA SNHG1(小核仁RNA宿主基因1)已被证明在HCC中起致癌作用,但其在RCD中除自噬和细胞凋亡外的功能尚不清楚。在此,我们根据癌症基因组图谱数据库的RNA测序数据,研究了SNHG1与五种RCD类型的156个典型标志物之间的相关性,并显示脱铁性贫血FANCD2(Fanconi贫血互补组D2)和G6PD(葡萄糖-6-磷酸脱氢酶)的负调控因子分别是与SNHG1相关性最高和第五高的因子。以生物信息学方法构建了SNHG1-miR-199a-5p/3p-FANCD2/G6PD竞争性内源性RNA网络。体外实验表明,在HCC细胞(Huh7和HepG2)中,miR-199a前体的过表达导致SNHG1、FANCD2和G6PD的表达降低,而SNHG1的敲低降低了FANCD2的表达,但增加了miR-199a-5p和miR-199a-3p的水平。此外,SNHG1的敲除增加了erastin介导的脱铁性贫血、铁积累和脂质过氧化。这些结果表明,SNHG1通过吸收miR-199a上调FANCD2和G6PD,从而抑制HCC中的脱铁性贫血。此外,基于SNHG1、FANCD2和G6PD表达的信号被鉴定为与HCC的总生存率和免疫微环境相关。总之,本研究确定了HCC中的SNHG1-miR-199a-FANCD2/G6PD轴,这是该肿瘤预后和治疗的潜在标志物。
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LncRNA SNHG1 upregulates FANCD2 and G6PD to suppress ferroptosis by sponging miR-199a-5p/3p in hepatocellular carcinoma.

Ferroptosis is a form of regulated cell death (RCD) triggered by iron-dependent lipid peroxidation and is closely associated with the occurrence and progression of hepatocellular carcinoma (HCC). The lncRNA SNHG1 (small nucleolar RNA host gene 1) has been shown to play an oncogenic role in HCC, but its function in RCD other than autophagy and apoptosis is still unknown. Here, we investigated the correlation between SNHG1 and 156 typical markers of five RCD types based on RNA sequencing data from The Cancer Genome Atlas database and showed the negative regulators of ferroptosis FANCD2 (Fanconi anemia complementation group D2) and G6PD (glucose-6-phosphate dehydrogenase) to be the most highly and fifth most highly correlating factors with SNHG1, respectively. A competitive endogenous RNA network of SNHG1 - miR-199a-5p/3p - FANCD2/G6PD was constructed bioinformatically. In vitro experiments showed that overexpression of the miR-199a precursor led to a decrease in expression of SNHG1, FANCD2, and G6PD, whereas knockdown of SNHG1 decreased expression of FANCD2 and G6PD but increased levels of miR-199a-5p and miR-199a-3p in HCC cells (Huh7 and HepG2). In addition, knockdown of SNHG1 increased erastin-mediated ferroptosis, iron accumulation, and lipid peroxidation. These results suggest that SNHG1 upregulates FANCD2 and G6PD by sponging miR-199a, thereby inhibiting ferroptosis in HCC. Moreover, a signature based on expression of SNHG1, FANCD2, and G6PD was identified as being associated with overall survival and the immunological microenvironment in HCC. Collectively, this study identified the SNHG1-miR-199a-FANCD2/G6PD axis in HCC, which is a potential marker for the prognosis and therapy of this tumor.

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来源期刊
Drug Discoveries and Therapeutics
Drug Discoveries and Therapeutics PHARMACOLOGY & PHARMACY-
CiteScore
3.20
自引率
3.20%
发文量
51
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