NSUN2依靠ALYREF调节Nrf2介导的氧化应激,减轻Dox诱导的肝损伤

IF 5.7 2区 生物学 Q1 BIOLOGY Biology Direct Pub Date : 2024-04-29 DOI:10.1186/s13062-024-00477-y
Yingying Huang, Xiao Li, Lin Wei, Shinan Ma, Liming Ma, Yuxin Zan, Xiju He, Yijun Tang, Yan Ding
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引用次数: 0

摘要

多柔比星(Dox)与各种肝损伤有关,限制了其临床应用。本研究探讨了NSUN2是否参与了Dox诱导的肝损伤及其相关分子机制。研究人员根据Dox疗法构建了体内和体外肝细胞损伤模型。通过Western印迹评估了NSUN2和氧化应激指标Nrf2、HO-1和NQO1的蛋白水平。通过 RNA 甲基化免疫沉淀(RIP)检测了 RNA 结合潜力。此外,还使用 RNA 荧光探针评估了 NSUN2 对 Nrf2 mRNA 合成和定位的影响。在Dox组中,NSUN2被下调,肝组织遭受了明显的病理损伤。ALT和AST水平明显升高。NSUN2干扰加剧了Dox诱导的肝细胞损伤,而NSUN2过表达可逆转这种损伤。RIP表明,NSUN2能识别Nrf2 mRNA并与之结合。Western印迹分析显示,NSUN2-WT组的Nrf2蛋白水平明显高于对照组,而突变体NSUN2组的Nrf2水平无明显变化。荧光素酶分析表明,NSUN2能识别并激活LO2细胞的Nrf2 5′UTR区域。此外,RIP分析显示,ALYREF能识别并结合Nrf2 mRNA,ALYREF能控制NSUN2对Nrf2的调控作用。NSUN2通过增加Nrf2 mRNA m5C甲基化来抑制抗氧化应激,从而调节Dox诱导的肝细胞损伤。NSUN2 对 Nrf2 的调节作用取决于 ALYREF。
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NSUN2 relies on ALYREF to regulate Nrf2-mediated oxidative stress and alleviate Dox-induced liver injury
Doxorubicin (Dox) is associated with various liver injuries, limiting its clinical utility. This study investigates whether NSUN2 participates in Dox-induced liver injury and the associated molecular mechanism. In vivo and in vitro liver cell injury models were constructed based on Dox therapy. The protein levels of NSUN2 and oxidative stress indicators Nrf2, HO-1, and NQO1 were evaluated by Western blot. The RNA binding potential was detected by RNA methylation immunoprecipitation (RIP). Additionally, the effect of NSUN2 on Nrf2 mRNA synthesis and localization was evaluated using an RNA fluorescence probe. NSUN2 was downregulated, and liver tissue suffered significant pathological damage in the Dox group. The levels of ALT and AST significantly increased. NSUN2 interference exacerbated Dox-induced liver cell damage, which was reversed by NSUN2 overexpression. RIP demonstrated that NSUN2 recognized and bound to Nrf2 mRNA. Western blot analysis showed the protein level of Nrf2 in the NSUN2-WT group was significantly higher than that of the control group, whereas there was no significant change in Nrf2 level in the mutant NSUN2 group. Luciferase analysis demonstrated that NSUN2 could recognize and activate the Nrf2 5′UTR region of LO2 cells. In addition, RIP analysis revealed that ALYREF could recognize and bind to Nrf2 mRNA and that ALYREF controls the regulatory effect of NSUN2 on Nrf2. NSUN2 regulates Dox-induced liver cell damage by increasing Nrf2 mRNA m5C methylation to inhibit inhibiting antioxidant stress. The regulatory effect of NSUN2 on Nrf2 depends on ALYREF.
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来源期刊
Biology Direct
Biology Direct 生物-生物学
CiteScore
6.40
自引率
10.90%
发文量
32
审稿时长
7 months
期刊介绍: Biology Direct serves the life science research community as an open access, peer-reviewed online journal, providing authors and readers with an alternative to the traditional model of peer review. Biology Direct considers original research articles, hypotheses, comments, discovery notes and reviews in subject areas currently identified as those most conducive to the open review approach, primarily those with a significant non-experimental component.
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