Gene: TREM2 ×
Source: BEFREE ×
Variant Gene Risk Allele Score vda Association Type Original DB Sentence supporting the association PMID PMID Year
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Our results support the consensus that the R47H variant is significantly associated with AD. 31513029

2020
dbSNP: rs766647311
rs766647311
TREM2 ; TREML1 ; LOC105375056
0.010 GeneticVariation BEFREE Our results, suggest that a p.(Gly145Trp)-induced structural disturbance and functional impairment of TREM2 may contribute to the pathogenesis of an AD-like form of dementia. 31464095

2020
dbSNP: rs766647311
rs766647311
TREM2 ; TREML1 ; LOC105375056
0.010 GeneticVariation BEFREE In a whole-exome sequencing study of a family with probable AD-type dementia without pathogenic variants in known autosomal dominant dementia disease genes and negative for the apolipoprotein E (APOE) ε4 allele, we identified an extremely rare TREM2 coding variant, that is, a glycine-to-tryptophan substitution at amino acid position 145 (NM_018965.3:c.433G>T/p.[Gly145Trp]). 31464095

2020
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs143332484
rs143332484
TREM2 ; LOC105375056
0.740 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs143332484
rs143332484
TREM2 ; LOC105375056
0.740 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs143332484
rs143332484
TREM2 ; LOC105375056
0.740 GeneticVariation BEFREE However, the isoform which lacks the 5' exon, but includes the transmembrane domain, was significantly lower in TREM2- p.R62H carriers than in AD cases (p = 0.007). 31068200

2019
dbSNP: rs2234255
rs2234255
TREM2 ; TREML1 ; LOC105375056
0.050 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs104894002
rs104894002
TREM2 ; LOC105375056
0.020 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs2234253
rs2234253
TREM2 ; LOC105375056
0.020 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs142232675
rs142232675
TREM2 ; LOC105375056
0.010 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs2234256
rs2234256
TREM2 ; TREML1 ; LOC105375056
0.010 GeneticVariation BEFREE Three variants in TREM2 (rs75932628 (R47H), rs2234255 (H157Y), and rs143332484 (R62H)) were significantly associated with AD risk, but the similar associations between rs104894002 (Q33X), rs2234253 (T96K), rs142232675 (D87N), rs2234256 (L211P), and AD were not proven. 30883352

2019
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Lymphoblast-derived integration-free iPSC line AD-TREM2-3 from a 74 year-old Alzheimer's disease patient expressing the TREM2 p.R47H variant. 29902745

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Molecular basis for the loss-of-function effects of the Alzheimer's disease-associated R47H variant of the immune receptor TREM2. 29794134

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE The rare variant R47H TREM2 is associated with an increased risk for Alzheimer's disease, supporting the hypothesis that TREM2 loss of function may exacerbate disease progression. 29599291

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Mouse models accurately reproducing phenotypes observed in Alzheimer' disease patients carrying the R47H coding variant are required to understand the TREM2 related dysfunctions responsible for the enhanced risk for late onset Alzheimer's disease. 30185230

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Moreover, the rare TREM2 variant (p.Arg47His), which was considered to be a risk factor for Alzheimer's disease in European descent populations, was not detected in our cohort. 29723869

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE These data suggest that the AD-associated TREM2 R47H variant increases risk for AD by conferring a loss of TREM2 function and enhancing neuritic dystrophy around plaques. 29859094

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE We generated transgenic mice expressing human CV or R47H TREM2 and lacking endogenous TREM2 in the 5XFAD AD model. 29321225

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Lymphoblast-derived integration-free iPSC line AD-TREM2-1 from a 67year-old Alzheimer's disease patient expressing the TREM2 p.R47H variant. 29602048

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Two DS cases had the AD-associated TREM2-R47H mutation, which manifested a morphologically extreme phenotype of megakaryocytes and erythrocytes in addition to impaired trafficking of TREM2 to the erythroid membrane. 29278889

2018
dbSNP: rs2234253
rs2234253
TREM2 ; LOC105375056
0.020 GeneticVariation BEFREE We identified 4 previously reported nonsynonymous variants (p.Asp39Glu, p.Arg62His, p.Thr96Lys, and p.Val126Gly) and 1 novel synonymous variant (p.Gln109Gln), none of which was significantly associated with the risk of Alzheimer's disease. 29723869

2018
dbSNP: rs121908402
rs121908402
TREM2 ; LOC105375056
0.010 GeneticVariation BEFREE We identified 4 previously reported nonsynonymous variants (p.Asp39Glu, p.Arg62His, p.Thr96Lys, and p.Val126Gly) and 1 novel synonymous variant (p.Gln109Gln), none of which was significantly associated with the risk of Alzheimer's disease. 29723869

2018
dbSNP: rs753325601
rs753325601
TREM2 ; LOC105375056
0.010 GeneticVariation BEFREE Given recent findings of enrichment of rare TREM2 variants (including R47C) in Alzheimer's disease, it is notable that we detected a homozygous TREM2 R47C carrier presenting with an FTD rather than an Alzheimer's disease phenotype. 29748150

2018
dbSNP: rs75932628
rs75932628
TREM2 ; LOC105375056
0.900 GeneticVariation BEFREE Shedding is not altered for the R47H-mutated TREM2 protein that confers an increased risk for the development of Alzheimers disease. 28923481

2017