弗雷明汉心脏研究中循环 CD34+CD133+ 内皮祖细胞与阿尔茨海默病风险降低之间的关系

Q4 Biochemistry, Genetics and Molecular Biology
Yixuan Wang, Jinghan Huang, T. F. Ang, Yibo Zhu, Q. Tao, Jesse B. Mez, M. Alosco, Gerald V. Denis, A. Belkina, A. Gurnani, Mark Ross, Bin Gong, Jingyan Han, Kathryn L. Lunetta, T. Stein, Rhoda Au, Lindsay A. Farrer, Xiaoling Zhang, Wei Qiao Qiu
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引用次数: 0

摘要

目的:内皮功能障碍与脑血管病变和阿尔茨海默病(AD)有关。然而,循环内皮细胞与阿尔茨海默病风险之间的联系仍不确定。我们的目的是利用弗雷明汉心脏研究的数据,研究各种循环内皮细胞亚型及其与阿尔茨海默病风险的潜在相关性。研究方法研究采用 Cox 比例危险回归和线性回归方法进行数据分析。此外,还进行了全基因组关联研究(GWAS)以进一步探索数据。研究结果在11种不同的循环内皮亚型中,只有表达CD34+CD133+的循环内皮祖细胞(EPCs)与AD风险的降低呈剂量依赖性的负相关。即使在调整了年龄、性别、受教育年限、载脂蛋白E(APOE)ε4状态和各种血管疾病后,这种关联依然存在。尤其值得注意的是,在高血压和脑微小出血患者中观察到了显著的相关性。同样,CD34+CD133+ EPCs 与特定脑区之间也发现了正相关,如循环 CD34+CD133+ 细胞比例越高,白质和海马体积越大。此外,一项GWAS研究揭示,CD34+CD133+细胞对AD风险的影响尤其体现在两个干细胞相关基因变异的同源基因型个体中:Kirre like nephrin family adhesion molecule 3(KIRREL3,rs580382 CC和rs4144611 TT)和exocyst complex component 6B(EXOC6B,rs61619102 CC)。结论研究结果表明,循环 CD34+CD133+ EPCs 具有保护作用,可为 AD 提供新的治疗途径,尤其是对血管病变患者和携带 KIRREL3 和 EXOC6B 基因特定基因型的患者。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The association between circulating CD34+CD133+ endothelial progenitor cells and reduced risk of Alzheimer’s disease in the Framingham Heart Study
Aim: Endothelial dysfunction has been associated with both cerebrovascular pathology and Alzheimer’s disease (AD). However, the connection between circulating endothelial cells and the risk of AD remains uncertain. The objective was to leverage data from the Framingham Heart Study to investigate various circulating endothelial subtypes and their potential correlations with the risk of AD. Methods: The study conducted data analyses using Cox proportional hazard regression and linear regression methods. Additionally, genome-wide association study (GWAS) was carried out to further explore the data. Results: Among the eleven distinct circulating endothelial subtypes, only circulating endothelial progenitor cells (EPCs) expressing CD34+CD133+ were found to be negatively and dose-dependently associated with reduced AD risk. This association persisted even after adjusting for age, sex, years of education, apolipoprotein E (APOE) ε4 status, and various vascular diseases. Particularly noteworthy was the significant association observed in individuals with hypertension and cerebral microbleeds. Consistently, positive associations were identified between CD34+CD133+ EPCs and specific brain regions, such as higher proportions of circulating CD34+CD133+ cells correlating with increased volumes of white matter and the hippocampus. Additionally, a GWAS study unveiled that CD34+CD133+ cells influenced AD risk specifically in individuals with homozygous genotypes for variants in two stem cell-related genes: kirre like nephrin family adhesion molecule 3 (KIRREL3, rs580382 CC and rs4144611 TT) and exocyst complex component 6B (EXOC6B, rs61619102 CC). Conclusions: The findings suggest that circulating CD34+CD133+ EPCs possess a protective effect and may offer a new therapeutic avenue for AD, especially in individuals with vascular pathology and those carrying specific genotypes of KIRREL3 and EXOC6B genes.
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