Alzheimer’s Disease variant portal (ADVP): a catalog of genetic findings for Alzheimer’s Disease

Kuksa, Pavel P.; Liu, Chia‐Lun; Fu, Wei; Qu, Liming; Zhao, Yi; Katanić, Živadin; Kuzma, Amanda B.; Ho, Pei‐Chuan; Tzeng, Kai‐Teh; Valladares, Otto; Naj, Adam C.; Schellenberg, Gerard D.; Wang, Li-San; Leung, Yuk Yee

doi:10.1101/2020.09.29.20203950

Cited by 2 publications

(1 citation statement)

References 60 publications

(105 reference statements)

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“…12 Also in the same locus is OAS2, which was independently shown to be associated with Alzheimer's disease. 95,96 Recent work has identified other SNPs close to this locus associated with severe responses to COVID-19 that also act as eQTLs and regulate the expression of OAS1, OAS3 and other distal genes such as DTX1. 32,33,97 Indeed, a series of different variants have been identified within OAS1 that modify susceptibility to infection with SARS-CoV-2, other viruses such as hepatitis C, developing type 1 diabetes, and multiple sclerosis; these variants have been proposed to cause amino acid changes, altered splicing (spliceQTLs) and altered expression (eQTLs).…”

Section: Discussionmentioning

confidence: 99%

A genetic link between risk for Alzheimer's disease and severe COVID-19 outcomes via the OAS1 gene

Magusali

Graham

Piers

et al. 2021

Brain

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Recently, we reported oligoadenylate synthetase 1 (OAS1) contributed to the risk of Alzheimer’s disease, by its enrichment in transcriptional networks expressed by microglia. However, the function of OAS1 within microglia was not known. Using genotyping from 1313 individuals with sporadic Alzheimer’s disease and 1234 control individuals, we confirm the OAS1 variant, rs1131454, is associated with increased risk for Alzheimer’s disease. The same OAS1 locus has been recently associated with severe coronavirus disease 2019 (COVID-19) outcomes, linking risk for both diseases. The single nucleotide polymorphisms rs1131454(A) and rs4766676(T) are associated with Alzheimer’s disease, and rs10735079(A) and rs6489867(T) are associated with severe COVID-19, where the risk alleles are linked with decreased OAS1 expression. Analysing single-cell RNA-sequencing data of myeloid cells from Alzheimer’s disease and COVID-19 patients, we identify co-expression networks containing interferon (IFN)-responsive genes, including OAS1, which are significantly upregulated with age and both diseases. In human induced pluripotent stem cell-derived microglia with lowered OAS1 expression, we show exaggerated production of TNF-α with IFN-γ stimulation, indicating OAS1 is required to limit the pro-inflammatory response of myeloid cells. Collectively, our data support a link between genetic risk for Alzheimer’s disease and susceptibility to critical illness with COVID-19 centred on OAS1, a finding with potential implications for future treatments of Alzheimer’s disease and COVID-19, and development of biomarkers to track disease progression.

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Section: Discussionmentioning

confidence: 99%

A genetic link between risk for Alzheimer's disease and severe COVID-19 outcomes via the OAS1 gene

Magusali

Graham

Piers

et al. 2021

Brain

View full text Add to dashboard Cite

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Genetic variability associated withOAS1expression in myeloid cells increases the risk of Alzheimer’s disease and severe COVID-19 outcomes

Magusali

et al. 2021

Preprint

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Genome-wide association studies of late-onset Alzheimer’s disease (AD) have highlighted the importance of variants associated with genes expressed by the innate immune system in determining risk for AD. Recently, we and others have shown that genes associated with variants that confer risk for AD are significantly enriched in transcriptional networks expressed by amyloid-responsive microglia. This allowed us to predict new risk genes for AD, including the interferon-responsive oligoadenylate synthetase 1 (OAS1). However, the function of OAS1 within microglia and its genetic pathway are not known. Using genotyping from 1,313 individuals with sporadic AD and 1,234 control individuals, we confirm that the OAS1 variant, rs1131454, is associated with increased risk for AD and decreased OAS1 expression. Moreover, we note that the same locus was recently associated with critical illness in response to COVID-19, linking variants that are associated with AD and a severe response to COVID-19. By analysing single-cell RNA-sequencing (scRNA-seq) data of isolated microglia from APPNL-G-F knock-in and wild-type C57BL/6J mice, we identify a transcriptional network that is significantly upregulated with age and amyloid deposition, and contains the mouse orthologue Oas1a, providing evidence that Oas1a plays an age-dependent function in the innate immune system. We identify a similar interferon-related transcriptional network containing OAS1 by analysing scRNA-seq data from human microglia isolated from individuals with AD. Finally, using human iPSC-derived microglial cells (h-iPSC-Mg), we see that OAS1 is required to limit the pro-inflammatory response of microglia. When stimulated with interferon-gamma (IFN-γ), we note that cells with lower OAS1 expression show an exaggerated pro-inflammatory response, with increased expression and secretion of TNF-α. Collectively, our data support a link between genetic risk for AD and susceptibility to critical illness with COVID-19 centred on OAS1 and interferon signalling, a finding with potential implications for future treatments of both AD and COVID-19, and the development of biomarkers to track disease progression.

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Alzheimer’s Disease variant portal (ADVP): a catalog of genetic findings for Alzheimer’s Disease

Cited by 2 publications

References 60 publications

A genetic link between risk for Alzheimer's disease and severe COVID-19 outcomes via the OAS1 gene

A genetic link between risk for Alzheimer's disease and severe COVID-19 outcomes via the OAS1 gene

Genetic variability associated withOAS1expression in myeloid cells increases the risk of Alzheimer’s disease and severe COVID-19 outcomes

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