阿尔茨海默病大脑颞中回的铁蛋白沉积、M6A 和免疫检查点相关基因表达

Qinfeng Liu , Fan Yang , Sijia Wu , Kai Yuan , Liyu Huang , Suping Cai
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摘要

阿尔茨海默病(AD)是一种常见的与遗传有关的认知障碍。研究表明,铁蛋白、N⁶-甲基腺苷(M6A)和免疫检查点与阿尔茨海默病的发病有关。然而,这三种基因通路对AD进展的影响仍不清楚。在此,我们利用在颞中回(MTG)表达的基因研究了97例阿尔茨海默病和98例正常对照组(NC)中铁突变、M6A和免疫检查点相关基因的差异。然后,我们对铁蛋白、M6A和免疫检查点相关基因的表达水平进行了相关分析,以探讨这些基因与阿尔茨海默病的关系。与NC相比,MTG在AD中的基因表达情况如下:(1)在铁变态反应相关基因中,CARS、CDKN1A、HSPB1、MT1G、EMC2、SAT1和SLC1A5的表达增加,而ACSL4、ATP5MC3、CSID1、CS、DPP4、GLS2和GPX4的表达减少;(2)在 M6A 相关基因中,HNRNPA2B1、IGF2BP2、RBM15B 和 YTHDC1 的表达增加,而 FTO、YTHDC2 和 YTHDF2 的表达减少;(3)免疫检查点相关基因(包括 CTLA4、HAVCR2 和 LAG3)的表达增加。此外,我们还通过文献综述确定了这些基因之间的相关基因通路。通过验证数据集,我们可以很好地验证我们的结果,并证明我们的结果具有良好的鲁棒性。我们通过基因表达得出结论:在AD发育过程中,MTG中的一整套铁变态反应、M6A和免疫检查点调控机制被激活。
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Ferroptosis, M6A and immune checkpoint-related gene expression in the middle temporal gyrus of the Alzheimer's disease brain

Alzheimer's disease (AD) is a common genetically related cognitive disorder. Studies have shown that ferroptosis, N⁶-Methyladenosine (M6A) and immune checkpoint are related to the development of AD. However, the effects of these three gene pathways on AD progression are still unclear. Here, we used genes expressed in the middle temporal gyrus (MTG) to study the differences in ferroptosis, M6A and immune checkpoint-related gene in 97 Alzheimer's disease and 98 normal controls (NC). We then conducted correlation analysis between ferroptosis, M6A and immune checkpoint-related gene expression levels to investigate the relationship between these genes and AD. Compared to the NC, the gene expression from MTG in AD are as follows: (1) in ferroptosis related genes, the expression of CARS, CDKN1A, HSPB1, MT1G, EMC2, SAT1 and SLC1A5 was increased, while the expression of ACSL4, ATP5MC3, CSID1, CS, DPP4, GLS2 and GPX4 was decreased; (2) in M6A-related genes, the expression of HNRNPA2B1, IGF2BP2, RBM15B and YTHDC1 was increased, while the expression of FTO, YTHDC2 and YTHDF2 was decreased; (3) the expression of immune checkpoint-related genes (including CTLA4, HAVCR2 and LAG3) was increased. Further, we determined related gene pathways among these genes by conducting a literature review. By verifying the dataset, we can well verify our results and prove that our results have good robustness. We concluded of gene expression that a complete set of ferroptosis, M6A and immune checkpoint regulatory mechanisms is activated in the MTG during AD development.

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