Intestinal Epithelial Cell-specific Knockout of METTL3 Aggravates Intestinal Inflammation in CLP Mice by Weakening the Intestinal Barrier.

IF 2.2 4区医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Current pharmaceutical biotechnology Pub Date : 2025-01-01 DOI:10.2174/0113892010271970240202054245

Hongzhou Shi, Jiahui Sun, Yaya Sun, Junjie Wu, Guangqing Jiang, Zhaiyue Xu, Xin Shi, Miao Fang

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Abstract

Background: Many studies have demonstrated that the expression of methyltransferase- like 3 (METTL3) is altered in various inflammatory diseases. Its specific mechanistic role in the intestinal inflammatory response during sepsis remains limited and requires further investigation.

Objectives: Explore the potential mechanism of METTL3 in the intestinal inflammatory response during sepsis.

Materials and methods: Immunohistochemical analysis was utilized to detect the expression of METTL3 in the necrotic intestine of patients with intestinal necrosis and the small intestine of cecal ligation and puncture (CLP) mice. Mice were subjected to the CLP and Sham surgeries, intestine tissue was harvested and performed HE staining, and ELISA to examine intestinal inflammatory responses, while TUNEL staining was applied to detect intestinal cell apoptosis. Additionally, ELISA was used to detect diamine oxidase (DAO) and intestinal fatty acid binding protein (I-FABP) levels in intestinal tissue. Immunohistochemistry and RT-qPCR were also employed to examine the mRNA and protein expression levels of Zona Occludens 1 (ZO-1) and Claudin-1. Finally, transcriptomic sequencing was performed on the small intestine tissues of METTL3 Knock-out (KO) and Wild-type (WT) mice in response to sepsis.

Results: METTL3 exhibited lower expression level in the necrotic intestine of patients and the small intestine of CLP mice. Loss of METTL3 in CLP mice triggered significantly higher expression of TNF-α and IL-18, down-regulated expression of ZO-1 and claudin-1, and decreased expression of DAO and I-FABP in the intestinal tissue. KEGG enrichment analysis showed that the differential genes were significantly enriched in immune-related pathways.

Conclusion: This study reveals a novel mechanism responsible for exacerbated intestinal inflammation orchestrated by METTL3. Particularly, METTL3 null mice displayed decreased ZO- 1 and Claudin-1 expression, which largely hampered intestinal epithelial barrier function, resulting in bacterial and toxin translocation and intestinal immune activation and inflammation against sepsis.

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肠上皮细胞特异性敲除 METTL3 会削弱肠屏障，从而加重 CLP 小鼠的肠道炎症。

背景：许多研究表明，类似甲基转移酶3（METTL3）的表达在各种炎症性疾病中发生了改变。其在败血症期间肠道炎症反应中的具体机制作用仍然有限，需要进一步研究：探索 METTL3 在败血症期间肠道炎症反应中的潜在机制：利用免疫组化分析检测METTL3在肠坏死患者坏死肠道和盲肠结扎穿刺（CLP）小鼠小肠中的表达。对小鼠进行CLP手术和Sham手术，收获肠组织并进行HE染色和ELISA检测肠道炎症反应，同时应用TUNEL染色检测肠道细胞凋亡。此外，还使用 ELISA 检测肠组织中二胺氧化酶（DAO）和肠脂肪酸结合蛋白（I-FABP）的水平。免疫组化和 RT-qPCR 被用来检测 Zona Occludens 1 (ZO-1) 和 Claudin-1 的 mRNA 和蛋白表达水平。最后，对METTL3基因敲除（KO）小鼠和野生型（WT）小鼠的小肠组织对败血症的反应进行了转录组测序：结果：METTL3在患者坏死肠道和CLP小鼠小肠中的表达水平较低。METTL3在CLP小鼠中缺失后，肠组织中TNF-α和IL-18的表达明显升高，ZO-1和claudin-1的表达下调，DAO和I-FABP的表达降低。KEGG富集分析表明，差异基因明显富集于免疫相关通路：结论：本研究揭示了 METTL3 导致肠道炎症加剧的新机制。结论：本研究揭示了 METTL3 导致肠道炎症加剧的新机制，特别是 METTL3 空腹小鼠 ZO- 1 和 Claudin-1 表达减少，这在很大程度上阻碍了肠上皮屏障功能，导致细菌和毒素转运以及肠道免疫激活和炎症，从而引发败血症。

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

Current pharmaceutical biotechnology 医学-生化与分子生物学

CiteScore

5.60

自引率

3.60%

发文量

203

审稿时长

6 months

期刊介绍： Current Pharmaceutical Biotechnology aims to cover all the latest and outstanding developments in Pharmaceutical Biotechnology. Each issue of the journal includes timely in-depth reviews, original research articles and letters written by leaders in the field, covering a range of current topics in scientific areas of Pharmaceutical Biotechnology. Invited and unsolicited review articles are welcome. The journal encourages contributions describing research at the interface of drug discovery and pharmacological applications, involving in vitro investigations and pre-clinical or clinical studies. Scientific areas within the scope of the journal include pharmaceutical chemistry, biochemistry and genetics, molecular and cellular biology, and polymer and materials sciences as they relate to pharmaceutical science and biotechnology. In addition, the journal also considers comprehensive studies and research advances pertaining food chemistry with pharmaceutical implication. Areas of interest include: DNA/protein engineering and processing Synthetic biotechnology Omics (genomics, proteomics, metabolomics and systems biology) Therapeutic biotechnology (gene therapy, peptide inhibitors, enzymes) Drug delivery and targeting Nanobiotechnology Molecular pharmaceutics and molecular pharmacology Analytical biotechnology (biosensing, advanced technology for detection of bioanalytes) Pharmacokinetics and pharmacodynamics Applied Microbiology Bioinformatics (computational biopharmaceutics and modeling) Environmental biotechnology Regenerative medicine (stem cells, tissue engineering and biomaterials) Translational immunology (cell therapies, antibody engineering, xenotransplantation) Industrial bioprocesses for drug production and development Biosafety Biotech ethics Special Issues devoted to crucial topics, providing the latest comprehensive information on cutting-edge areas of research and technological advances, are welcome. Current Pharmaceutical Biotechnology is an essential journal for academic, clinical, government and pharmaceutical scientists who wish to be kept informed and up-to-date with the latest and most important developments.