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

Yang, Hongtian; Onos, Kristen D.; Choi, Kwangbom; Keezer, Kelly J.; Skelly, Daniel A.; Carter, Gregory W.; Howell, Gareth R.

doi:10.1101/2020.06.02.130237

Cited by 8 publications

(19 citation statements)

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“…1f). This observation is consistent with the previous report that accumulation of Aβ plaques leads to activation of the interferon pathway [27][28][29][30] . The expression of interferon pathway-related genes was robust in Tau4RΔK-AP microglia but was not observed in Tau4RΔK microglia, suggesting that both Aβ plaques and tau aggregation are necessary to fully induce EADAM differentiation.…”

Section: Identification Of a Novel Early-stage Ad-associated Microglia (Eadam) Triggered By Both Aβ Plaques And Tau Depositionsupporting

confidence: 94%

“…LADAM continues to express classic DAM genes but also upregulates additional genes, including Cd74 and MHC Class II genes. These broad LADAM marker-expressing microglia (Cd74 and MHC Class II genes) have been previously shown in some amyloidosis mouse models at late stages (known as activated response microglia) [27][28][29] , but these genes are likely to be contributed by mild tau phosphorylation shown in these amyloidosis mouse models, based on our findings from Tau4RΔK (Fig. 2).…”

Section: Discussion: Discovery Of Novel Disease Stage-specific Microglial Subtypes Induced By Aβ Plaques and Tau Pathologysupporting

confidence: 61%

“…EADAM are characterized by many interferon-pathway-related genes (Ifit3, Ifit204, Ifit2) and interferon regulating transcription factors (Irf2/7/9) as well as inflammatory chemokines (Ccl12, Cxcl10, Ccl5, Ccl2). Some of the genes in EADAM have been observed in other mouse models of amyloidosis that show early AD-like pathology [27][28][29] , including APP;PS1 and 5xFAD. However, given that EADAM-enriched genes are expressed in much higher levels in our Tau4RΔK-AP microglia, this strongly supports the view that both Aβ and tau pathologies are required to induce disease stage-specific microglia subtypes in AD.…”

Section: Discussion: Discovery Of Novel Disease Stage-specific Microglial Subtypes Induced By Aβ Plaques and Tau Pathologymentioning

confidence: 99%

“…These datasets show that tau pathologies are sufficient to trigger the emergence of LADAM and that their amplification is Aβ plaque-dependent. However, since MHC class II genes that are expressed in LADAM, such as Cd74, H2-A2, H2-Eb1, and H2-Ab1 have also been previously observed in microglia in the CK-p25 neurodegeneration mouse model 31,32 and also in some mouse models of late stage amyloidosis [27][28][29] , LADAM may be induced at least in part by neuronal death.…”

Section: Identification Of Late-stage Ad-associated Microglia (Ladam)mentioning

confidence: 93%

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Amyloid-beta and tau pathologies are both necessary to induce novel stage-specific microglia subtypes during Alzheimer’s disease progression

Kim

Wei

et al. 2021

Preprint

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It is unknown whether specific microglia are selectively induced by amyloid-β(Aβ), tau pathologies, or both in combination. To address this, we use single-cell RNA-sequencing to profile mice bearing both Aβ and tau pathologies during Alzheimer's disease (AD). We identify novel microglia subtypes induced in a disease stage-specific manner. We show that during early-stage disease, interferon signaling induces a subtype of microglia termed EADAM. During late-stage disease, a second microglia subtype termed LADAM is detected. While EADAM and LADAM-like microglia are observed in other neurodegenerative models, the magnitude and composition of subtype markers are distinct from microglia observed with AD-like pathology. The pattern of EADAM- and LADAM-associated gene expression is observed in microglia from human AD, during the early and late stages of disease, respectively. Furthermore, we observe that several siglec genes are selectively expressed in either EADAM or LADAM. Siglecg is expressed in white-matter-associated LADAM, and expression of the human orthologue of Siglecg is progressively elevated in AD-stage-dependent manner but not shown in non-AD tauopathy. Our findings imply that both Aβ and tau pathologies are required for disease stage-specific induction of EADAM and LADAM.

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Section: Identification Of a Novel Early-stage Ad-associated Microglia (Eadam) Triggered By Both Aβ Plaques And Tau Depositionsupporting

confidence: 94%

Section: Discussion: Discovery Of Novel Disease Stage-specific Microglial Subtypes Induced By Aβ Plaques and Tau Pathologysupporting

confidence: 61%

Section: Discussion: Discovery Of Novel Disease Stage-specific Microglial Subtypes Induced By Aβ Plaques and Tau Pathologymentioning

confidence: 99%

Section: Identification Of Late-stage Ad-associated Microglia (Ladam)mentioning

confidence: 93%

See 2 more Smart Citations

Amyloid-beta and tau pathologies are both necessary to induce novel stage-specific microglia subtypes during Alzheimer’s disease progression

Kim

Wei

et al. 2021

Preprint

View full text Add to dashboard Cite

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“…Genetic variation, or differences in genetic background, can have a major influence on vascular biology (Bjorkegren & Lusis, 2022; De Silva, Modrick, et al, 2018; von Scheidt et al, 2017; Yang et al, 2021). Rather than basing all conclusions on a single genetic strain, we used mice on two very different genetic backgrounds.…”

Section: Discussionmentioning

confidence: 99%

Angiotensin II‐induced endothelial dysfunction: Impact of sex, genetic background, and rho kinase

Kinzenbaw

Langmack

Faraci

2022

Physiological Reports

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The renin‐angiotensin system (RAS) contributes to vascular disease with multiple cardiovascular risk factors including hypertension. As a major effector within the RAS, angiotensin II (Ang II) activates diverse signaling mechanisms that affect vascular biology. Despite the impact of such vascular pathophysiology, our understanding of the effects of Ang II in relation to the function of endothelial cells is incomplete. Because genetic background and biological sex can be determinants of vascular disease, we performed studies examining the direct effects of Ang II using carotid arteries from male and female mice on two genetic backgrounds, C57BL/6J and FVB/NJ. Although FVB/NJ mice are much less susceptible to atherosclerosis than C57BL/6J, the effects of Ang II on endothelial cells in FVB/NJ are poorly defined. Overnight incubation of isolated arteries with Ang II (10 nmol/L), impaired endothelial function in both strains and sexes by approximately one‐half ( p < 0.05). To examine the potential mechanistic contribution of Rho kinase (ROCK), we treated arteries with SLX‐2119, an inhibitor with high selectivity for ROCK2. In both male and female mice of both strains, SLX‐2119 largely restored endothelial function to normal, compared to vessels treated with vehicle. Thus, Ang II‐induced endothelial dysfunction was observed in both FVB/NJ and C57BL/6J mice. This effect was sex‐independent. In all groups, effects of Ang II were reversed by inhibition of ROCK2 with SLX‐2119. These studies provide the first evidence that ROCK2 may be a key contributor to Ang II‐induced endothelial dysfunction in both sexes and in mouse strains that differ in relation to other major aspects of vascular disease.

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Integrating transcriptomic datasets across neurological disease identifies unique myeloid subpopulations driving disease‐specific signatures

Wishart

Spiteri

Locatelli

et al. 2022

Glia

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Microglia and bone marrow-derived monocytes are key elements of central nervous system (CNS) inflammation, both capable of enhancing and dampening immunemediated pathology. However, the study-specific focus on individual cell types, disease models or experimental approaches has limited our ability to infer common and disease-specific responses. This meta-analysis integrates bulk and single-cell transcriptomic datasets of microglia and monocytes from disease models of autoimmunity, neurodegeneration, sterile injury, and infection to build a comprehensive resource connecting myeloid responses across CNS disease. We demonstrate that the bulk microglial and monocyte program is highly contingent on the disease environment, challenging the notion of a universal microglial disease signature. Integration of six single-cell RNA-sequencing datasets revealed that these disease-specific signatures are likely driven by differing proportions of unique myeloid subpopulations that were individually expanded in different disease settings. These subsets were functionally-defined as neurodegeneration-associated, inflammatory, interferonresponsive, phagocytic, antigen-presenting, and lipopolysaccharide-responsive cellular states, revealing a core set of myeloid responses at the single-cell level that are conserved across CNS pathology. Showcasing the predictive and practical value of this resource, we performed differential expression analysis on microglia and

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

Cited by 8 publications

References 50 publications

Amyloid-beta and tau pathologies are both necessary to induce novel stage-specific microglia subtypes during Alzheimer’s disease progression

Amyloid-beta and tau pathologies are both necessary to induce novel stage-specific microglia subtypes during Alzheimer’s disease progression

Angiotensin II‐induced endothelial dysfunction: Impact of sex, genetic background, and rho kinase

Integrating transcriptomic datasets across neurological disease identifies unique myeloid subpopulations driving disease‐specific signatures

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