GWAS on family history of Alzheimer’s disease

Marioni, Riccardo E.; Harris, Sarah E.; Zhang, Qian; McRae, Allan F.; Hagenaars, Saskia P.; Hill, W. David; Davies, Gail; Ritchie, Craig W.; Gale, Catharine R.; Starr, John M.; Goate, Alison; Porteous, David J.; Yang, Jian; Evans, Kathryn; Deary, Ian J.; Wray, Naomi R.; Visscher, Peter M.

doi:10.1038/s41398-018-0150-6

Cited by 451 publications

(547 citation statements)

References 34 publications

(46 reference statements)

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“…We obtained in total 63 modules (). GSEA with the GWAS gene set generated from Marioni et al (), at different cut‐offs for statistical significance as explained above (Fig A and ), demonstrated that the largest set of risk genes (e.g., n = 1,799 genes at P mar < 0.05) enrich among 4 APPtg‐ and TAUtg‐based modules (Turquoise, Blue, Fig A and ). However, when taking gene sets defined by increasing statistical significance ( P mar < 0.001 or smaller), the only module that persistently demonstrates significant enrichment with GWAS genes is the APPtg‐Blue module (see Fig A).…”

Section: Resultsmentioning

confidence: 90%

“…In the genotype comparison, mRNA expression in all transgenic (TG) mice is compared to all wild‐type (WT) mice. In the age*genotype comparison, we assess which transcripts are differentially expressed in the 10M TG mice compared to all other groups. DBased on Marioni et al (), various sets of AD GWAS risk genes were created using different cut‐off P ‐values indicated on the x ‐axis (number of genes within each set is written in gray). Enrichment for AD risk genes was assessed among the different statistical comparisons for APPtg and TAUtg mice (A*G: age*genotype, Gen: genotype), using gene set enrichment analysis (GSEA, Subramanian et al , ).…”

Section: Resultsmentioning

confidence: 99%

“…We included established AD risk variants, i.e., loci with P < 5 × 10e‐8 in various GWAS studies, as well as subthreshold AD risk variants as these contribute significantly to AD risk predictions through polygenic inheritance (Escott‐Price et al , , ). We examined multiple sets of such genes taken from Marioni et al (), which combines UK Biobank AD‐by‐proxy data with the IGAP database and which confers risk loci onto genes based on proximity (thus from here on, AD risk variants are referred to as AD risk genes, noticing that this is based on these assumptions). Using arbitrary Bonferroni‐adjusted P ‐value ( P mar ) cut‐offs with decreasing significance for AD association, gene sets of increasing size were created (see Fig D and ).…”

Section: Resultsmentioning

confidence: 99%

“… AGene set enrichment analysis using Fisher's exact test of GWAS genes from Marioni et al () at different P ‐value cut‐offs among the WGCNA‐derived modules in APPtg or TAUtg mice (see also ). Colors represent −log10 (Benjamini–Yekutieli‐adjusted P ‐value) for the enrichment.…”

Section: Resultsmentioning

confidence: 99%

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Novel Alzheimer risk genes determine the microglia response to amyloid‐β but not to TAU pathology

et al. 2020

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Polygenic risk scores have identified that genetic variants without genome‐wide significance still add to the genetic risk of developing Alzheimer's disease (AD). Whether and how subthreshold risk loci translate into relevant disease pathways is unknown. We investigate here the involvement of AD risk variants in the transcriptional responses of two mouse models: APPswe/PS1L166P and Thy‐TAU22. A unique gene expression module, highly enriched for AD risk genes, is specifically responsive to Aβ but not TAU pathology. We identify in this module 7 established AD risk genes (APOE, CLU, INPP5D, CD33, PLCG2, SPI1, and FCER1G) and 11 AD GWAS genes below the genome‐wide significance threshold (GPC2, TREML2, SYK, GRN, SLC2A5, SAMSN1, PYDC1, HEXB, RRBP1, LYN, and BLNK), that become significantly upregulated when exposed to Aβ. Single microglia sequencing confirms that Aβ, not TAU, pathology induces marked transcriptional changes in microglia, including increased proportions of activated microglia. We conclude that genetic risk of AD functionally translates into different microglia pathway responses to Aβ pathology, placing AD genetic risk downstream of the amyloid pathway but upstream of TAU pathology.

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Section: Resultsmentioning

confidence: 90%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Novel Alzheimer risk genes determine the microglia response to amyloid‐β but not to TAU pathology

et al. 2020

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“…The lower association signal for the 17q22 locus in the UK biobank cohort could be explained by differences in case ascertainment of AD. In the UK biobank, Alzheimer dementia is ascertained via self‐report information from family history (parent or a first‐degree relative with AD or dementia) as a proxy‐phenotype for the participants (Marioni et al, ). This method relies on people to provide accurate information about whether their parents developed AD, for which misclassification of case status is of greater concern than consortia relying upon clinician‐reported diagnoses.…”

Section: Discussionmentioning

confidence: 99%

A functional variant in the miR‐142 promoter modulating its expression and conferring risk of Alzheimer disease

Ghanbari

Munshi

et al. 2019

Human Mutation

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Noncoding RNAs have been widely recognized as essential mediators of gene regulation. However, in contrast to protein‐coding genes, much less is known about the influence of noncoding RNAs on human diseases. Here we examined the association of genetic variants located in primary microRNA sequences and long noncoding RNAs (lncRNAs) with Alzheimer disease (AD) by leveraging data from the largest genome‐wide association meta‐analysis of late‐onset AD. Variants annotated to 5 miRNAs and 10 lncRNAs (in seven distinct loci) exceeded the Bonferroni‐corrected significance threshold (p < 1.02 × 10−6). Among these, a leading variant (rs2526377:A>G) at the 17q22 locus annotated to two noncoding RNAs (MIR142 and BZRAP1‐AS) was significantly associated with a reduced risk of AD and fulfilled predefined criteria for being a functional variant. Our functional genomic analyses revealed that rs2526377 affects the promoter activity and decreases the expression of miR‐142. Moreover, differential expression analysis by RNA‐Seq in human iPSC‐derived neural progenitor cells and the hippocampus of miR‐142 knockout mice demonstrated multiple target genes of miR‐142 in the brain that are likely to be involved in the inflammatory and neurodegenerative manifestations of AD. These include TGFBR1 and PICALM, of which their derepression in the brain due to reduced expression levels of miR‐142‐3p may reduce the risk of AD.

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Genetic Complexities of Cerebral Small Vessel Disease, Blood Pressure, and Dementia

Sargurupremraj,

Soumaré,

Bis

et al. 2024

JAMA Netw Open

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ImportanceVascular disease is a treatable contributor to dementia risk, but the role of specific markers remains unclear, making prevention strategies uncertain.ObjectiveTo investigate the causal association between white matter hyperintensity (WMH) burden, clinical stroke, blood pressure (BP), and dementia risk, while accounting for potential epidemiologic biases.Design, Setting, and ParticipantsThis study first examined the association of genetically determined WMH burden, stroke, and BP levels with Alzheimer disease (AD) in a 2-sample mendelian randomization (2SMR) framework. Second, using population-based studies (1979-2018) with prospective dementia surveillance, the genetic association of WMH, stroke, and BP with incident all-cause dementia was examined. Data analysis was performed from July 26, 2020, through July 24, 2022.ExposuresGenetically determined WMH burden and BP levels, as well as genetic liability to stroke derived from genome-wide association studies (GWASs) in European ancestry populations.Main Outcomes and MeasuresThe association of genetic instruments for WMH, stroke, and BP with dementia was studied using GWASs of AD (defined clinically and additionally meta-analyzed including both clinically diagnosed AD and AD defined based on parental history [AD-meta]) for 2SMR and incident all-cause dementia for longitudinal analyses.ResultsIn 2SMR (summary statistics–based) analyses using AD GWASs with up to 75 024 AD cases (mean [SD] age at AD onset, 75.5 [4.4] years; 56.9% women), larger WMH burden showed evidence for a causal association with increased risk of AD (odds ratio [OR], 1.43; 95% CI, 1.10-1.86; P = .007, per unit increase in WMH risk alleles) and AD-meta (OR, 1.19; 95% CI, 1.06-1.34; P = .008), after accounting for pulse pressure for the former. Blood pressure traits showed evidence for a protective association with AD, with evidence for confounding by shared genetic instruments. In the longitudinal (individual-level data) analyses involving 10 699 incident all-cause dementia cases (mean [SD] age at dementia diagnosis, 74.4 [9.1] years; 55.4% women), no significant association was observed between larger WMH burden and incident all-cause dementia (hazard ratio [HR], 1.02; 95% CI, 1.00-1.04; P = .07). Although all exposures were associated with mortality, with the strongest association observed for systolic BP (HR, 1.04; 95% CI, 1.03-1.06; P = 1.9 × 10−14), there was no evidence for selective survival bias during follow-up using illness-death models. In secondary analyses using polygenic scores, the association of genetic liability to stroke, but not genetically determined WMH, with dementia outcomes was attenuated after adjusting for interim stroke.ConclusionsThese findings suggest that WMH is a primary vascular factor associated with dementia risk, emphasizing its significance in preventive strategies for dementia. Future studies are warranted to examine whether this finding can be generalized to non-European populations.

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GWAS on family history of Alzheimer’s disease

Cited by 451 publications

References 34 publications

Novel Alzheimer risk genes determine the microglia response to amyloid‐β but not to TAU pathology

Novel Alzheimer risk genes determine the microglia response to amyloid‐β but not to TAU pathology

A functional variant in the miR‐142 promoter modulating its expression and conferring risk of Alzheimer disease

Genetic Complexities of Cerebral Small Vessel Disease, Blood Pressure, and Dementia

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