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More evidence for association of a rare TREM2 mutation (R47H) with Alzheimer's disease risk.


ABSTRACT: Over 20 risk loci have been identified for late-onset Alzheimer's disease (LOAD), most of which display relatively small effect sizes. Recently, a rare missense (R47H) variant, rs75932628 in TREM2, has been shown to mediate LOAD risk substantially in Icelandic and Caucasian populations. Here, we present more evidence for the association of the R47H with LOAD risk in a Caucasian population comprising 4567 LOAD cases and controls. Our results show that carriers of the R47H variant have a significantly increased risk for LOAD (odds ratio = 7.40, p = 3.66E-06). In addition to Alzheimer's disease risk, we also examined the association of R47H with Alzheimer's disease-related phenotypes, including age-at-onset, psychosis, and amyloid deposition but found no significant association. Our results corroborate those of other studies implicating TREM2 as an LOAD risk locus and indicate the need to determine its biological role in the context of neurodegeneration.

SUBMITTER: Rosenthal SL 

PROVIDER: S-EPMC4465085 | biostudies-literature | 2015 Aug

REPOSITORIES: biostudies-literature

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More evidence for association of a rare TREM2 mutation (R47H) with Alzheimer's disease risk.

Rosenthal Samantha L SL   Bamne Mikhil N MN   Wang Xingbin X   Berman Sarah S   Snitz Beth E BE   Klunk William E WE   Sweet Robert A RA   Demirci F Yesim FY   Lopez Oscar L OL   Kamboh M Ilyas MI  

Neurobiology of aging 20150425 8


Over 20 risk loci have been identified for late-onset Alzheimer's disease (LOAD), most of which display relatively small effect sizes. Recently, a rare missense (R47H) variant, rs75932628 in TREM2, has been shown to mediate LOAD risk substantially in Icelandic and Caucasian populations. Here, we present more evidence for the association of the R47H with LOAD risk in a Caucasian population comprising 4567 LOAD cases and controls. Our results show that carriers of the R47H variant have a significa  ...[more]

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