Co-localized SNPs Affecting the Expression of Taste Perception Genes are linked to Alzheimer's Disease

Paule Valery Joseph, Malak Abbas, Gabriel Goodney, Ana Diallo, Amadou Gaye
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Abstract

Background While previous research has shown the potential links between taste perception pathways and brain-related conditions, the area involving Alzheimer's disease remains incompletely understood. Taste perception involves neurotransmitter signaling, including serotonin, glutamate, and dopamine. Disruptions in these pathways are implicated in neurodegenerative diseases. The integration of olfactory and taste signals in flavor perception may impact brain health, evident in olfactory dysfunction as an early symptom in neurodegenerative conditions. Shared immune response and inflammatory pathways may contribute to the association between altered taste perception and conditions like neurodegeneration, present in Alzheimer's disease. Methods This study consists of an exploration of expression-quantitative trait loci (eQTL), utilizing whole-blood transcriptome profiles, of 28 taste perception genes, from a combined cohort of 475 African American subjects. This comprehensive dataset was subsequently intersected with single-nucleotide polymorphisms (SNPs) identified in Genome-Wide Association Studies (GWAS) of Alzheimer's Disease (AD). Finally, the investigation delved into assessing the association between eQTLs reported in GWAS of AD and the profiles of 741 proteins from the Olink Neurological Panel. Results The eQTL analysis unveiled 3,547 statistically significant SNP-Gene associations, involving 412 distinct SNPs that spanned all 28 taste genes. In 17 GWAS studies encompassing various traits, a total of 14 SNPs associated with 12 genes were identified, with three SNPs consistently linked to Alzheimer's disease across four GWAS studies. All three SNPs demonstrated significant associations with the down-regulation of TAS2R41, and two of them were additionally associated with the down-regulation of TAS2R60. In the subsequent pQTL analysis, two of the SNPs linked to TAS2R41 and TAS2R60 genes (rs117771145 and rs10228407) were correlated with the upregulation of two proteins, namely EPHB6 and ADGRB3. Conclusions Our investigation introduces a new perspective to the understanding of Alzheimer's disease, emphasizing the significance of bitter taste receptor genes in its pathogenesis. These discoveries set the stage for subsequent research to delve into these receptors as promising avenues for both intervention and diagnosis. Nevertheless, the translation of these genetic insights into clinical practice requires a more profound understanding of the implicated pathways and their pertinence to the disease's progression across diverse populations.
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影响味觉感知基因表达的共定位 SNP 与阿尔茨海默病有关
背景虽然先前的研究表明味觉通路与大脑相关疾病之间存在潜在联系,但对涉及阿尔茨海默氏症的领域仍不完全了解。味觉感知涉及神经递质信号传递,包括血清素、谷氨酸和多巴胺。这些通路的中断与神经退行性疾病有关。嗅觉和味觉信号在味觉感知中的整合可能会影响大脑健康,嗅觉功能障碍是神经退行性疾病的早期症状之一。本研究利用全血转录组图谱,对来自 475 名非洲裔美国人受试者的 28 个味觉基因的表达定量性状位点(eQTL)进行了探索。随后,该综合数据集与阿尔茨海默病(AD)全基因组关联研究(GWAS)中发现的单核苷酸多态性(SNPs)进行了交叉分析。最后,调查还深入评估了在阿尔茨海默病 GWAS 中报告的 eQTL 与 Olink 神经系统面板中的 741 种蛋白质之间的关联。结果eQTL 分析揭示了 3,547 个具有统计学意义的 SNP 基因关联,涉及 412 个不同的 SNP,涵盖了所有 28 个味觉基因。在包含各种性状的 17 项 GWAS 研究中,共发现了与 12 个基因相关的 14 个 SNPs,其中有 3 个 SNPs 在 4 项 GWAS 研究中始终与阿尔茨海默病相关。这三个SNP都与TAS2R41的下调有显著关联,其中两个还与TAS2R60的下调有额外关联。在随后的 pQTL 分析中,与 TAS2R41 和 TAS2R60 基因相关的 SNPs 中的两个(rs117771145 和 rs10228407)与 EPHB6 和 ADGRB3 这两种蛋白质的上调相关。这些发现为后续研究奠定了基础,以便深入研究这些受体,为干预和诊断提供有希望的途径。然而,要将这些基因研究成果转化为临床实践,还需要更深入地了解与之相关的途径及其与不同人群疾病进展的相关性。
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