The Correlation Analysis Between m6A Methylation Modification and Ferroptosis Induced by Cigarette Smoke in Human Bronchial Epithelium

IF 3.1 4区医学 Q3 IMMUNOLOGY Immunity, Inflammation and Disease Pub Date : 2024-12-17 DOI:10.1002/iid3.70104

Xiaomei Duan, Tingting Hu, Lijuan Xu, Zheng Li, Jing Jing, Dan Xu, Jianbing Ding, Fengsen Li, Min Jiang, Jing Wang

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Abstract

Background

Chronic obstructive pulmonary disease (COPD), a prevalent respiratory condition, is characterized by long-term airway inflammation, which can lead to airway remodeling and persistent airflow restriction. Exposure to cigarette smoke is known as a major contributor to COPD development. Research has confirmed that ferroptosis and m6A modification are closely related to various inflammatory-related diseases. However, the correlation between m6A methylation and ferroptosis in COPD has not been confirmed. In this study, combined with bioinformatics analysis and molecular biology methods we investigated how m6A methylation was correlated to ferroptosis-associated genes (SLC7A11 and NQO-1) in cigarette smoke induced 16HBES cells.

Methods

Two microarray datasets (GSE30063 and GSE64614) were combined to identify differentially expressed genes (DEGs) through the application of bioinformatics techniques. A cigarette smoke (CS)-induced 16HBE cells model was established. The ROS, GSH, MDA, and total iron content were detected by relevant detection kits. The expression levels associated with ferroptosis and m6A methylation modification-related genes were determined via reverse transcription-quantitative polymerase chain reaction and western blot.

Results

Overall, 529 DEGs were identified in the above two databases. For COPD patients, significant changes were observed in FAGs (GCLC, NQO-1, SLC7A11) and m6A methylation-related genes (FTO). A negative correlation was also noted between the expression level of genes linked to ferroptosis (SLC7A11 and NQO-1) and that of the m6A methylation gene (FTO). The in vitro experiments results indicate that SLC7A11 and NQO-1 were significantly downregulated, and FTO were significantly upregulated. In addition, cigarette smoke stimulation increased the levels of MDA, LPO, and ROS, while reducing the content of GSH and total iron content in 16HBE cells.

Conclusion

Our findings explored the relationship between ferroptosis and m6A methylation in COPD, and screened out SLC7A11, NQO-1 and FTO may be critical in the pathogenesis of COPD.

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m6A甲基化修饰与吸烟致人支气管上皮铁下垂的相关性分析。

背景：慢性阻塞性肺疾病（COPD）是一种常见的呼吸系统疾病，其特点是气道长期炎症，可导致气道重塑和持续气流受限。众所周知，接触香烟烟雾是导致慢性阻塞性肺病的主要因素。研究证实，铁蛋白沉积和 m6A 修饰与各种炎症相关疾病密切相关。然而，慢性阻塞性肺病中 m6A 甲基化与铁变态反应之间的相关性尚未得到证实。在本研究中，我们结合生物信息学分析和分子生物学方法，研究了在香烟烟雾诱导的 16HBES 细胞中，m6A 甲基化与铁变态反应相关基因（SLC7A11 和 NQO-1）的相关性：方法：结合两个微阵列数据集（GSE30063 和 GSE64614），应用生物信息学技术识别差异表达基因（DEGs）。建立了香烟烟雾（CS）诱导的 16HBE 细胞模型。通过相关检测试剂盒检测了ROS、GSH、MDA和总铁含量。通过逆转录-定量聚合酶链反应和免疫印迹法测定与铁变态反应和 m6A 甲基化修饰相关基因的表达水平：结果：上述两个数据库共鉴定出 529 个 DEGs。慢性阻塞性肺病患者的 FAGs（GCLC、NQO-1、SLC7A11）和 m6A 甲基化相关基因（FTO）发生了显著变化。此外，还发现与铁变态反应有关的基因（SLC7A11 和 NQO-1）的表达水平与 m6A 甲基化基因（FTO）的表达水平呈负相关。体外实验结果表明，SLC7A11 和 NQO-1 的表达明显下调，而 FTO 的表达明显上调。此外，香烟烟雾刺激增加了 16HBE 细胞中 MDA、LPO 和 ROS 的水平，同时降低了 GSH 和总铁的含量：结论：我们的研究结果探讨了慢性阻塞性肺病中的铁变态反应与 m6A 甲基化之间的关系，并筛选出 SLC7A11、NQO-1 和 FTO 可能在慢性阻塞性肺病的发病机制中起关键作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Immunity, Inflammation and Disease Medicine-Immunology and Allergy

CiteScore

3.60

自引率

0.00%

发文量

146

审稿时长

8 weeks

期刊介绍： Immunity, Inflammation and Disease is a peer-reviewed, open access, interdisciplinary journal providing rapid publication of research across the broad field of immunology. Immunity, Inflammation and Disease gives rapid consideration to papers in all areas of clinical and basic research. The journal is indexed in Medline and the Science Citation Index Expanded (part of Web of Science), among others. It welcomes original work that enhances the understanding of immunology in areas including: • cellular and molecular immunology • clinical immunology • allergy • immunochemistry • immunogenetics • immune signalling • immune development • imaging • mathematical modelling • autoimmunity • transplantation immunology • cancer immunology