Common variants in Alzheimer’s disease: Novel association of six genetic variants with AD and risk stratification by polygenic risk scores

Rojas, Itziar de; Moreno‐Grau, Sonia; Tesi, Niccolò; Grenier‐Boley, Benjamin; Andrade, Víctor; Jansen, Iris E.; Pedersen, Nancy L.; Stringa, Najada; Zettergren, Anna; Hernández, Isabel; Montrreal, Laura; Antúnez, Carmen; Antonell, Anna; Tankard, Rick M.; Bis, Joshua C.; Sims, Rebecca; Bellenguez, Céline; Quintela, Inés; González‐Pérez, Antonio; Calero, Miguel; Franco, Emilio; Macı́as, Juan; Blesa, Rafael; Menéndez-González, Manuel; Frank-García, Ana; Royo, José Luís; Moreno, Fermín; Huerto, Raquel; Baquero, Miquel; Díez-Fairén, Mónica; Lage, Carmen; García-Madrona, Sebastián; García, Pablo; Alarcón‐Martín, Emilio; Valero, Sergi; Sotolongo-Grau, Óscar; Consortia, Pgc-Alz; García‐Ribas, Guillermo; Sánchez‐Juan, Pascual; Pástor, Pau; Pérez‐Tur, Jordi; Piñol‐Ripoll, Gerard; Munáin, Adolfo López de; García‐Alberca, José María; Bullido, María J.; Álvarez, Victoria; Lleó, Alberto; Real, Luís Miguel; Mir, Pablo; Medina, Miguel Á.; Scheltens, Philip; Holstege, Henne; Marquié, Marta; Sáez, María Eugenia; Carracedo, Ángel; Amouyel, Philippe; Williams, Julie; Seshadri, Sudha; Duijn, Cornelia M. van; Mather, Karen A.; Sánchez‐Valle, Raquel; Serrano-Rı́os, Manuel; Orellana, Adelina; Tárraga, Lluís; Blennow, Kaj; Huisman, Martijn; Andreassen, Ole A.; Posthuma, Daniëlle; Clarimón, Jordi; Boada, Merçé; Flier, Wiesje M. van der; Ramı́rez, Alfredo; Lambert, Jean‐Charles; Lee, Sven J. van der; Ruiz, Agustín

doi:10.1101/19012021

Cited by 26 publications

(55 citation statements)

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“…In recent years, genome-wide association studies (GWASs) reinforce that AD is a complex disease, in which APP processing and immune response play key roles [212]. Whole genome sequencing (WGS), GWAS, and gene-expression network analysis proved that LOAD genetics implicates microglial pathways and CR1, SII1, MS4As, TREM2, ABCA7, CD33, INPP5D genes are associated with disease risk [212]. The results of the largest meta-GWAS approach (analyzing 19,089 AD cases) and follow-up analysis for AD risk has been published very recently [212].…”

Section: Genetic Risk Factors Of Ad: Classical Studies and Novel Resultsmentioning

confidence: 99%

“…Whole genome sequencing (WGS), GWAS, and gene-expression network analysis proved that LOAD genetics implicates microglial pathways and CR1, SII1, MS4As, TREM2, ABCA7, CD33, INPP5D genes are associated with disease risk [212]. The results of the largest meta-GWAS approach (analyzing 19,089 AD cases) and follow-up analysis for AD risk has been published very recently [212]. It was found that altogether 39 genetic variants may be associated with AD risk (beyond the APOE variants).…”

Section: Genetic Risk Factors Of Ad: Classical Studies and Novel Resultsmentioning

confidence: 99%

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Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

2020

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The structural polymorphism and the physiological and pathophysiological roles of two important proteins, β-amyloid (Aβ) and tau, that play a key role in Alzheimer’s disease (AD) are reviewed. Recent results demonstrate that monomeric Aβ has important physiological functions. Toxic oligomeric Aβ assemblies (AβOs) may play a decisive role in AD pathogenesis. The polymorph fibrillar Aβ (fAβ) form has a very ordered cross-β structure and is assumed to be non-toxic. Tau monomers also have several important physiological actions; however, their oligomerization leads to toxic oligomers (TauOs). Further polymerization results in probably non-toxic fibrillar structures, among others neurofibrillary tangles (NFTs). Their structure was determined by cryo-electron microscopy at atomic level. Both AβOs and TauOs may initiate neurodegenerative processes, and their interactions and crosstalk determine the pathophysiological changes in AD. TauOs (perhaps also AβO) have prionoid character, and they may be responsible for cell-to-cell spreading of the disease. Both extra- and intracellular AβOs and TauOs (and not the previously hypothesized amyloid plaques and NFTs) may represent the novel targets of AD drug research.

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Section: Genetic Risk Factors Of Ad: Classical Studies and Novel Resultsmentioning

confidence: 99%

Section: Genetic Risk Factors Of Ad: Classical Studies and Novel Resultsmentioning

confidence: 99%

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

2020

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“…However, previous studies to determine roles of GWAS genes in AD have primarily been limited to the B6 genetic background. Therefore, we aimed to determine whether our wild-derived AD panel provided an enhanced platform to study human-relevant AD genes using a panel of 54 GWAS genes identified in two recent meta-analyses ( Supplementary Table 6 ) 31,32 . A total of 36 microglia-relevant genes were detectable across our panel.…”

Section: Resultsmentioning

confidence: 99%

“…The human AD GWAS genes were selected from two recent meta-analyses (Table 1 31 and Table S2 32 ). The GWAS genes from both tables were combined and were overlapped with equivalent mouse genes in scRNA-seq data from this study.…”

Section: Methodsmentioning

confidence: 99%

Natural genetic variation determines microglia heterogeneity in wild-derived mouse models of Alzheimer’s disease

Yang

Onos

Choi

et al. 2020

Preprint

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Microglia are now considered drivers of Alzheimer's disease (AD) pathology. However, single-cell RNA-sequencing (scRNA-seq) of microglia in mice, a key preclinical model organsim, have shown mixed results regarding translatability to human studies. To address this, scRNA-seq of microglia from C57BL/6J (B6) and wild-derived strains WSB/EiJ, CAST/EiJ and PWK/PhJ carrying APP/PS1 was performed and demonstrated that genetic diversity significantly altered features and dynamics of microglia in baseline neuroimmune functions and in response to amyloidosis. There was significant variation in abundance of microglial subpopulations, including numbers of disease-associated microglia and interferon-responding microglia across the strains.Further, for each subpopulation, significant gene expression differences were observed between strains, and relative to B6 that included nineteen genes previously associated with human AD including Apoe, Trem2, Bin1 and Sorl1. This resource will be critical in the development of appropriately targeted therapeutics for AD and a range of other neurological diseases. 30 Introduction 31Alzheimer's disease (AD) is defined by the neuropathological accumulation of beta 32 amyloid plaques, neurofibrillary tangles of tau and widespread neuronal loss. AD is the 33 most common cause of adult dementia and is characterized by a wide range of 34 cognitive and behavioral deficits that severely impact quality of life and the ability to self-35 care. Recent work has re-focused the field towards the contribution of brain glial cells to 36 the initiation and spread of these disease-specific pathologies, and specifically on the 37 role of microglia as potentially a causative cell type in driving disease development and 38 progression. Human genome-wide association studies (GWAS) have identified more 39 than 25 variants near genes uniquely expressed in microglia that are predicted to 40 increase susceptibility for AD. In light of this complexity, the mouse represents a critical 41 model system to dissect the role of microglia and other glia in AD. 42 43There has been large debate regarding the alignment of mouse microglia to human 44 microglia in terms of identity, diversity and function. With the more widespread use of 45 single-cell sequencing technology, a number of groups have suggested that the species 46 difference is too great for conclusions drawn from mouse models to inform our 47 understanding of human microglia1,2. Central to this argument is the discovery and 48 description of a specific class of microglia in the mouse, disease-associated microglia 49 (DAM)3. Based upon the current data it is unclear whether the presence or absence of 50 DAM in human AD patients is the result of differences in tissue collection, extraction of 51 cells, genetic diversity of patients, sub-type of AD presented in donors or even the 52 relevant disease1,4. Recent work has demonstrated that single-nucleus RNA 53 sequencing of stored human tissue fails to detect differences in microglia activation 54 between AD and contro...

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“…Apolipoprotein ε4 allele (APOE4) is the only common high risk genetic variant (odds ratio (OR)=3.32) (11,12). Genome wide association studies (GWAS) have further identified many common genetic variants with low risk (OR=1.1-1.2) of which 40 have genome wide significance (12)(13)(14). Exome chip analyses have additionally yielded rare variants in the very same genes, i.e.…”

Section: The Heritability Of Admentioning

confidence: 99%

Translating genetic risk of Alzheimer’s disease into mechanistic insight and drug targets

Sierksma

Escott‐Price

Strooper

2020

Science

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To provide better prevention and treatment, we need to understand the environmental and genetic risks of Alzheimer’s disease (AD). However, the definition of AD has been confounded with dementia in many studies. Thus, overinterpretation of genetic findings with regard to mechanisms and drug targets may explain, in part, controversies in the field. Here, we analyze the different forms of genetic risk of AD and how these can be used to model disease. We stress the importance of studying gene variants in the right cell types and in the right pathological context. The lack of mechanistic understanding of genetic variation has become the major bottleneck in the search for new drug targets for AD.

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Common variants in Alzheimer’s disease: Novel association of six genetic variants with AD and risk stratification by polygenic risk scores

Cited by 26 publications

References 64 publications

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

Natural genetic variation determines microglia heterogeneity in wild-derived mouse models of Alzheimer’s disease

Translating genetic risk of Alzheimer’s disease into mechanistic insight and drug targets

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