Genome and epigenome wide studies of plasma protein biomarkers for Alzheimer’s disease implicate TBCA and TREM2 in disease risk

Author:

Hillary Robert F.ORCID,Gadd Danni A.ORCID,McCartney Daniel L.ORCID,Shi LiuORCID,Campbell ArchieORCID,Walker Rosie M.ORCID,Ritchie Craig W.ORCID,Deary Ian J.ORCID,Evans Kathryn L.ORCID,Nevado-Holgado Alejo J.ORCID,Hayward CarolineORCID,Porteous David J.ORCID,McIntosh Andrew M.ORCID,Lovestone SimonORCID,Robinson Matthew R.ORCID,Marioni Riccardo E.ORCID

Abstract

Abstract The levels of many blood proteins are associated with Alzheimer’s disease or its pathological hallmarks. Elucidating the molecular factors that control circulating levels of these proteins may help to identify proteins causally associated with the disease. Here, genome-wide and epigenome-wide studies (nindividuals≤1,064) were performed on plasma levels of 281 Alzheimer’s disease-associated proteins, identified by a systematic review of the literature. We quantified the contributions of genetic and epigenetic variation towards inter-individual variability in plasma protein levels. Sixty-one independent genetic and 32 epigenetic loci were associated with expression levels of 49 proteins; eight and 24 of these respective findings are previously unreported. Novel findings included an association between plasma TREM2 levels and a polymorphism and CpG site within the MS4A4A locus. Through Mendelian randomisation analyses, causal associations were observed between higher plasma TBCA and TREM2 levels and lower Alzheimer’s disease risk. Our data inform the regulation of biomarker levels and their relationships with Alzheimer’s disease.

Publisher

Cold Spring Harbor Laboratory

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