CD44和MAPK14介导的脱铁性贫血在失血性休克中的作用。

IF 6.1 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Haoran Ye, Shasha He, Yuan Du, Yuchen Wang, Yahui Hu, Chunxia Zhao, Yueting Jin, Fangyu Liu, Yuhong Guo
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引用次数: 0

摘要

阐明失血性休克中脱铁途径的诱导和关键基因的转录调控。R软件用于分析GSE64711数据集,分离与脱铁性贫血相关的基因。对富集分析和蛋白质相互作用网络进行了组装。使用WGCNA鉴定hub基因并与脱铁相关基因交叉,突出hub基因CD44和MAPK14。在大鼠失血性休克模型中,评估心脏ROS、Fe2+、MDA和GSH水平。通过蛋白质印迹法检测心肌组织中的关键脱铁蛋白(SLC7A11/GPX4)。免疫组化证实了中枢基因CD44和MAPK14的表达。分析GSE64711数据集发现337个差异表达基因,其中12个与脱铁性贫血有关。富集分析强调了与脱铁症密切相关的途径。利用Genemania,我们发现这些基因主要影响ROS代谢和氧化应激反应。WGCNA鉴定CD44和MAPK14为枢纽基因。大鼠心肌组织验证显示,失血性休克模型中存在显著的心脏损伤,ROS和MDA水平升高,GSH水平降低。在失血性休克大鼠模型中,脱铁途径SLC7A11/GPX4被激活,免疫组织化学显示CD44和MAPK14的表达水平显著增加。我们通过将生物信息学分析与体内实验相结合,证明了失血性休克中存在组织脱铁性贫血。具体而言,我们观察到SLC7A11/GPX4脱铁途径的激活。此外,CD44和MAPK14被鉴定为失血性休克的中枢基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Involvement of CD44 and MAPK14-mediated ferroptosis in hemorrhagic shock

Involvement of CD44 and MAPK14-mediated ferroptosis in hemorrhagic shock

To elucidate the induction of ferroptotic pathways and the transcriptional modulation of pivotal genes in the context of hemorrhagic shock. The R software was used to analyze the GSE64711 dataset, isolating genes relevant to ferroptosis. Enrichment analyses and protein interaction networks were assembled. Using WGCNA hub genes were identified and intersected with ferroptosis-related genes, highlighting hub genes CD44 and MAPK14. In a rat hemorrhagic shock model, cardiac ROS, Fe2+, MDA, and GSH levels were assessed. Key ferroptotic proteins (SLC7A11/GPX4) in myocardial tissues were examined via western blot. Hub genes, CD44 and MAPK14, expressions were confirmed through immunohistochemistry. Analyzing the GSE64711 dataset revealed 337 differentially expressed genes, including 12 linked to ferroptosis. Enrichment analysis highlighted pathways closely related to ferroptosis. Using Genemania, we found these genes mainly affect ROS metabolism and oxidative stress response. WGCNA identified CD44 and MAPK14 as hub genes. Rat myocardial tissue validation showed significant cardiac damage and elevated ROS and MDA levels, and decreased GSH levels in the hemorrhagic shock model. The ferroptotic pathway SLC7A11/GPX4 was activated, and immunohistochemistry showed a significant increase in the expression levels of CD44 and MAPK14 in the hemorrhagic shock rat model. We demonstrated the presence of tissue ferroptosis in hemorrhagic shock by combining bioinformatics analysis with in vivo experimentation. Specifically, we observed the activation of the SLC7A11/GPX4 ferroptotic pathway. Further, CD44 and MAPK14 were identified as hub genes in hemorrhagic shock.

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来源期刊
Apoptosis
Apoptosis 生物-生化与分子生物学
CiteScore
9.10
自引率
4.20%
发文量
85
审稿时长
1 months
期刊介绍: Apoptosis, a monthly international peer-reviewed journal, focuses on the rapid publication of innovative investigations into programmed cell death. The journal aims to stimulate research on the mechanisms and role of apoptosis in various human diseases, such as cancer, autoimmune disease, viral infection, AIDS, cardiovascular disease, neurodegenerative disorders, osteoporosis, and aging. The Editor-In-Chief acknowledges the importance of advancing clinical therapies for apoptosis-related diseases. Apoptosis considers Original Articles, Reviews, Short Communications, Letters to the Editor, and Book Reviews for publication.
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