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Spi1 剂量的适度变化揭示了改变小胶质细胞功能的潜力,这种改变在阿尔茨海默病中可见。

Modest changes in Spi1 dosage reveal the potential for altered microglial function as seen in Alzheimer's disease.

机构信息

Division of Infection and Immunity, Cardiff University, Cardiff, UK.

UK Dementia Research Institute at Cardiff, Cardiff University, Hadyn Ellis Building, Maindy Road, Cardiff, CF24 4HQ, UK.

出版信息

Sci Rep. 2021 Jul 22;11(1):14935. doi: 10.1038/s41598-021-94324-z.

Abstract

Genetic association studies have identified multiple variants at the SPI1 locus that modify risk and age of onset for Alzheimer's Disease (AD). Reports linking risk variants to gene expression suggest that variants denoting higher SPI1 expression are likely to have an earlier AD onset, and several other AD risk genes contain PU.1 binding sites in the promoter region. Overall, this suggests the level of SPI1 may alter microglial phenotype potentially impacting AD. This study determined how the microglial transcriptome was altered following modest changes to Spi1 expression in primary mouse microglia. RNA-sequencing was performed on microglia with reduced or increased Spi1/PU.1 expression to provide an unbiased approach to determine transcriptomic changes affected by Spi1. In summary, a reduction in microglial Spi1 resulted in the dysregulation of transcripts encoding proteins involved in DNA replication pathways while an increased Spi1 results in an upregulation of genes associated with immune response pathways. Additionally, a subset of 194 Spi1 dose-sensitive genes was identified and pathway analysis suggests that several innate immune and interferon response pathways are impacted by the concentration of Spi1. Together these results suggest Spi1 levels can alter the microglial transcriptome and suggests interferon pathways may be altered in individuals with AD related Spi1 risk SNPs.

摘要

遗传关联研究已经确定了 SPI1 基因座上的多个变体,这些变体可以改变阿尔茨海默病(AD)的风险和发病年龄。将风险变体与基因表达联系起来的报告表明,表达 SPI1 的变体较高的人可能会更早发病,并且其他几个 AD 风险基因在启动子区域包含 PU.1 结合位点。总的来说,这表明 SPI1 的水平可能会改变小胶质细胞表型,从而潜在地影响 AD。本研究确定了在原代小鼠小胶质细胞中 SPI1 表达适度改变后,小胶质细胞转录组是如何改变的。对表达减少或增加 Spi1/PU.1 的小胶质细胞进行 RNA 测序,提供了一种确定受 Spi1 影响的转录组变化的无偏方法。总的来说,小胶质细胞 Spi1 的减少导致编码参与 DNA 复制途径的蛋白质的转录本失调,而 Spi1 的增加导致与免疫反应途径相关的基因上调。此外,还鉴定出一组 194 个 Spi1 剂量敏感基因,通路分析表明,几种固有免疫和干扰素反应通路受到 Spi1 浓度的影响。这些结果表明 Spi1 水平可以改变小胶质细胞的转录组,并表明 AD 相关 Spi1 风险 SNPs 个体中的干扰素途径可能会发生改变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f973/8298495/0d9b79bb41b6/41598_2021_94324_Fig1_HTML.jpg

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