A Genome-wide Gene-Expression Analysis and Database in Transgenic Mice during Development of Amyloid or Tau Pathology

Matarı́n, Mar; Salih, Dervis A.; Yasvoina, Marina V.; Cummings, Damian M.; Guelfi, Sebastian; Liu, Wenfei; Solim, Muzammil A. Nahaboo; Moens, Thomas; Paublete, Rocio Moreno; Ali, Shabinah S.; Perona, Marina; Desai, Roshni A; Smith, Kenneth J.; Latcham, Judy; Fulleylove, Michael; Richardson, Jill C.; Hardy, John; Edwards, Frances A.

doi:10.1016/j.celrep.2014.12.041

Cited by 265 publications

(342 citation statements)

References 30 publications

(32 reference statements)

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“…The module preservation statistic (called "z-summary") combines multiple metrics that assess the conservation of co-expression patterns within a given module in a second (validation) dataset. As validation data, we employed four datasets: a) microarray gene expression data from cortex (DLPFC) from a previous study by Zhang and colleagues 46 , b) microarray gene expression data from mouse brain from a previous study by Matarin and colleagues 48 , c) an independent test dataset from the ROSMAP study (unpublished, data available from Synapse doi:10.7303/syn3388564) d) histone modification data (H3K9Ac chromatin immunoprecipitation followed by sequencing, unpublished, available doi:10.7303/syn4896408). We summarize the analyses of these data below.…”

Section: Replication Of Gene Modulesmentioning

confidence: 99%

A molecular network of the aging brain implicatesINPPL1andPLXNB1in Alzheimer’s disease

Mostafavi

Gaiteri

Sullivan

et al. 2017

Preprint

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One sentence summary: Molecular network analysis of RNA sequencing data from the aging human cortex identifies new Alzheimer's and cognitive decline genes.material for any purpose without crediting the original authors.was not peer-reviewed) in the Public Domain. It is no longer restricted by copyright. Anyone can legally share, reuse, remix, or adapt thisThe copyright holder has placed this preprint (which . http://dx.doi.org/10.1101/205807 doi: bioRxiv preprint first posted online 2 AbstractThe fact that only symptomatic therapies of small effect are available for Alzheimer's disease (AD) today highlights the need for new therapeutic targets with which to prevent a major contributor to aging-related cognitive decline. Here, we report the construction and validation of a molecular network of the aging human frontal cortex. Using RNA sequence data from 478 individuals, we first identify the role of modules of coexpressed genes, and then confirm them in independent AD datasets. Then, we prioritize influential genes in AD-related modules and test our predictions in human model systems. We functionally validate two putative regulator genes in human astrocytes: INPPL1 and PLXNB1, whose activity in AD may be related to semaphorin signalling and type II diabetes, which have both been implicated in AD. This arc of network identification followed by statistical and experimental validation provides specific new targets for therapeutic development and illustrates a network approach to a complex disease.

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Section: Replication Of Gene Modulesmentioning

confidence: 99%

A molecular network of the aging brain implicatesINPPL1andPLXNB1in Alzheimer’s disease

Mostafavi

Gaiteri

Sullivan

et al. 2017

Preprint

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show abstract

“…NAD is an essential co-enzyme for several biological process, such as cell death, energy metabolism and calcium mobilization. NMNAT2 is highly expressed in the brain, and along with axon protection following injury (44)(45)(46)(47)(48)(49) is implicated in neurodegenerative disease (50)(51)(52)(53). While functional genetics indicate PHR proteins can inhibit NMNAT2, the biochemical mechanism by which this occurs remains untested.…”

mentioning

confidence: 99%

PAM forms an atypical SCF ubiquitin ligase complex that ubiquitinates and degrades NMNAT2

Desbois

Crawley

Evans

et al. 2018

Journal of Biological Chemistry

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“…2016). Genetic evidence for this complexity comes from the identification of microglial response genes as risk loci for Alzheimer's disease (Matarin et al 2015) Guest Editorial 3 At a theoretical level, the negative outcome of anti-amyloid therapy was not excluded, even without putting the causal contribution of Aβ to AD into question (Karran et al 2011). In one disease scenario, Aβ was proposed as a driver of the disease process.…”

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confidence: 99%

Alzheimer’s disease: where next for anti-amyloid therapies?

Hardy¹,

Strooper²

2017

Brain

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A Genome-wide Gene-Expression Analysis and Database in Transgenic Mice during Development of Amyloid or Tau Pathology

Cited by 265 publications

References 30 publications

A molecular network of the aging brain implicatesINPPL1andPLXNB1in Alzheimer’s disease

A molecular network of the aging brain implicatesINPPL1andPLXNB1in Alzheimer’s disease

PAM forms an atypical SCF ubiquitin ligase complex that ubiquitinates and degrades NMNAT2

Alzheimer’s disease: where next for anti-amyloid therapies?

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