Proteo-genomics of soluble TREM2 in cerebrospinal fluid provides novel insights and identifies novel modulators for Alzheimer’s disease

特雷姆2 神经学 脑脊液 疾病 医学 神经科学 基因组学 人体生理学 阿尔茨海默病 分子医学 生物信息学 计算生物学 生物 病理 内科学 受体 遗传学 基因 基因组 髓系细胞 癌症 细胞周期
作者
Lihua Wang,Niko-Petteri Nykänen,Daniel Western,Priyanka Gorijala,Jigyasha Timsina,Fuhai Li,Zhaohua Wang,Muhammad Ali,Chengran Yang,Menghan Liu,William Brock,Marta Marquié,Merçé Boada,Ignacio Álvarez,Miquel Aguilar,Pau Pástor,Agustı́n Ruiz,Raquel Puerta,Adelina Orellana,Jarod Rutledge
出处
期刊:Molecular Neurodegeneration [BioMed Central]
卷期号:19 (1): 1-1 被引量:44
标识
DOI:10.1186/s13024-023-00687-4
摘要

Abstract Triggering receptor expressed on myeloid cells 2 (TREM2) plays a critical role in microglial activation, survival, and apoptosis, as well as in Alzheimer’s disease (AD) pathogenesis. We previously reported the MS4A locus as a key modulator for soluble TREM2 (sTREM2) in cerebrospinal fluid (CSF). To identify additional novel genetic modifiers of sTREM2, we performed the largest genome-wide association study (GWAS) and identified four loci for CSF sTREM2 in 3,350 individuals of European ancestry. Through multi-ethnic fine mapping, we identified two independent missense variants (p.M178V in MS4A4A and p.A112T in MS4A6A ) that drive the association in MS4A locus and showed an epistatic effect for sTREM2 levels and AD risk. The novel TREM2 locus on chr 6 contains two rare missense variants (rs75932628 p.R47H, P =7.16×10 -19 ; rs142232675 p.D87N, P =2.71×10 -10 ) associated with sTREM2 and AD risk. The third novel locus in the TGFBR2 and RBMS3 gene region (rs73823326, P =3.86×10 -9 ) included a regulatory variant with a microglia-specific chromatin loop for the promoter of TGFBR2 . Using cell-based assays we demonstrate that overexpression and knock-down of TGFBR2, but not RBMS3, leads to significant changes of sTREM2. The last novel locus is located on the APOE region (rs11666329, P =2.52×10 -8 ), but we demonstrated that this signal was independent of APOE genotype. This signal colocalized with cis-eQTL of NECTIN2 in the brain cortex and cis-pQTL of NECTIN2 in CSF. Overexpression of NECTIN2 led to an increase of sTREM2 supporting the genetic findings. To our knowledge, this is the largest study to date aimed at identifying genetic modifiers of CSF sTREM2. This study provided novel insights into the MS4A and TREM2 loci, two well-known AD risk genes, and identified TGFBR2 and NECTIN2 as additional modulators involved in TREM2 biology.
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