Deficiency of TYROBP, an adapter protein for TREM2 and CR3 receptors, is neuroprotective in a mouse model of early Alzheimer’s pathology

Haure‐Mirande, Jean‐Vianney; Audrain, Mickaël; Fanutza, Tomas; Kim, Soong Ho; Klein, William L.; Glabe, Charles G.; Readhead, Ben; Dudley, Joel T.; Blitzer, Robert D.; Wang, Minghui; Zhang, Bin; Schadt, Eric E.; Gandy, Sam; Ehrlich, Michelle E.

doi:10.1007/s00401-017-1737-3

Cited by 95 publications

(108 citation statements)

References 87 publications

(125 reference statements)

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“…In the present study, three cases of NHD showed the homozygous mutation of c.141delG in exon 3 of DAP12. A recent study showed that deficiency of DAP12 does not modify the number and size of Aβ plaque deposition in the prefrontal cortex and the hippocampus of APP/PSEN1 mice, although DAP12 deficiency reduces plaque compaction, microglial clustering, and phagocytosis (20). Furthermore, phosphorylation of tau is attenuated in female APP/ PSEN1 mice with loss of DAP12.…”

Section: Resultsmentioning

confidence: 99%

Alzheimer's disease pathology in Nasu-Hakola disease brains

Satoh

Kino

Yanaizu

et al. 2018

IRDR

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Section: Resultsmentioning

confidence: 99%

Alzheimer's disease pathology in Nasu-Hakola disease brains

Satoh

Kino

Yanaizu

et al. 2018

IRDR

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“…Loss of TREM2 in a tau mouse model led to less brain atrophy. Interestingly, deficiency of TYROBP, the adapter protein for TREM2, was neuroprotective in a mouse model of AD (Haure‐Mirande et al, ). The deficiency of TYROBP resulted in an altered expression of AD‐related genes, with less severe neuritic dystrophy and attenuated learning behavior deficits.…”

Section: Discussionmentioning

confidence: 99%

TREM2 triggers microglial density and age‐related neuronal loss

Linnartz‐Gerlach

Bodea

Klaus

et al. 2018

Glia

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The microglial triggering receptor expressed on myeloid cells 2 (TREM2) signals via the activatory membrane adaptor molecule TYROBP. Genetic variants or mutations of TREM2 or TYROBP have been linked to inflammatory neurodegenerative diseases associated with aging. The typical aging process goes along with microglial changes and mild neuronal loss, but the exact contribution of TREM2 is still unclear. Aged TREM2 knock‐out mice showed decreased age‐related neuronal loss in the substantia nigra and the hippocampus. Transcriptomic analysis of the brains of 24 months old TREM2 knock‐out mice revealed 211 differentially expressed genes mostly downregulated and associated with complement activation and oxidative stress response pathways. Consistently, 24 months old TREM2 knock‐out mice showed lower transcription of microglial ( Aif1 and Tmem119 ), oxidative stress markers ( Inos, Cyba, and Cybb ) and complement components ( C1qa, C1qb, C1qc, C3, C4b, Itgam, and Itgb2 ), decreased microglial numbers and expression of the microglial activation marker Cd68, as well as accumulation of oxidized lipids. Cultured microglia of TREM2 knock‐out mice showed reduced phagocytosis and oxidative burst. Thus, microglial TREM2 contributes to age‐related microglial changes, phagocytic oxidative burst, and loss of neurons with possible detrimental effects during physiological aging.

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“…Genes relating to TYROBP signaling, which is implicated in Alzheimer's and regulates phagocytosis, cell proliferation, activation and survival, were significantly upregulated (Keren-Shaul et al, 2017;Landreth & Reed-Geaghan, 2009;Ma et al, 2015). Substantiating these findings Tyrobp knockout mice models have proven to suppress inflammation in neurodegenerative models including Alzheimer's, thereby minimizing neuronal dystrophy, implicating a failure in the resolution of inflammation in Alzheimer's(Bakker et al, 2000;Haure-Mirande et al, 2017). Interestingly mutations and expression of downstream members are also linked with…”

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confidence: 99%

A core transcriptional signature of human microglia: Derivation and utility in describing region‐dependent alterations associated with Alzheimer's disease

Patir

Shih

McColl

et al. 2019

Glia

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Growing recognition of the pivotal role microglia play in neurodegenerative and neuroinflammatory disorders has accentuated the need to characterize their function in health and disease. Studies in mouse have applied transcriptome‐wide profiling of microglia to reveal key features of microglial ontogeny, functional profile, and phenotypic diversity. While similar, human microglia exhibit clear differences to their mouse counterparts, underlining the need to develop a better understanding of the human microglial profile. On examining published microglia gene signatures, limited consistency was observed between studies. Hence, we sought to derive a core microglia signature of the human central nervous system (CNS), through a comprehensive analysis of existing transcriptomic datasets. Nine datasets derived from cells and tissues, isolated from various regions of the CNS across numerous donors, were subjected independently to an unbiased correlation network analysis. From each dataset, a list of coexpressing genes corresponding to microglia was identified, with 249 genes highly conserved between them. This core signature included known microglial markers, and compared with other signatures provides a gene set specific to microglia in the context of the CNS. The utility of this signature was demonstrated by its use in detecting qualitative and quantitative region‐specific alterations in aging and Alzheimer's disease. These analyses highlighted the reactive response of microglia in vulnerable brain regions such as the entorhinal cortex and hippocampus, additionally implicating pathways associated with disease progression. We believe this resource and the analyses described here, will support further investigations to the contribution of human microglia in CNS health and disease.

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Deficiency of TYROBP, an adapter protein for TREM2 and CR3 receptors, is neuroprotective in a mouse model of early Alzheimer’s pathology

Cited by 95 publications

References 87 publications

Alzheimer's disease pathology in Nasu-Hakola disease brains

Alzheimer's disease pathology in Nasu-Hakola disease brains

TREM2 triggers microglial density and age‐related neuronal loss

A core transcriptional signature of human microglia: Derivation and utility in describing region‐dependent alterations associated with Alzheimer's disease

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