Ocular hypertension suppresses homeostatic gene expression in optic nerve head microglia of DBA/2 J mice

Tribble, James R.; Harder, Jeffrey M.; Williams, Pete A.; John, Simon W. M.

doi:10.1186/s13041-020-00603-7

Cited by 36 publications

(40 citation statements)

References 84 publications

(142 reference statements)

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“…Transcriptomic data from the DBA/2J mouse model of glaucoma suggest that early inflammation is driven by CD11b + CD11c + cells, while CD11b + CD11c − cells initially adopt an anti-inflammatory pattern of gene expression ( Tribble et al, 2020a ; Williams et al, 2019 ). Our results support this finding by demonstrating that CD11b + CD11c + cells upregulated IL-1α, TNF-α, and C1q expression prior to contribution from CD11b + CD11c − cells.…”

Section: Discussionmentioning

confidence: 99%

“…Results suggest that CD11b + CD11c + cells are early contributors to A1 astrocyte formation following IOP elevation (eIOP). Transcriptomic data from fluorescence-activated cell sorting (FACS)-isolated CD11b + CD11c + retinal cells in the DBA/2J mouse model of glaucoma demonstrate that this population is enriched for infiltrating macrophages compared to other blood-borne immune cells and resident microglia ( Tribble et al, 2020a ). It should be noted that the embryonic origin of the CD11b + CD11c + cell population has not been conclusively demonstrated, and these cells could therefore represent resident retinal microglia that have undergone a state change, infiltrating macrophages, or a mixture of both.…”

Section: Discussionmentioning

confidence: 99%

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GLP-1 Receptor Agonist NLY01 Reduces Retinal Inflammation and Neuron Death Secondary to Ocular Hypertension

et al. 2020

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SUMMARY Glaucoma is the leading cause of irreversible blindness and is characterized by the death of retinal ganglion cells (RGCs). Recent studies have implicated pro-inflammatory microglia, macrophages, and A1 astrocytes in the pathogenesis of neurodegenerative diseases. The role of pro-inflammatory, neurotoxic A1 astrocytes in glaucoma is just beginning to be explored. Using a mouse model of glaucoma, we demonstrate that ocular hypertension is sufficient to trigger production of C1q, interleukin-1α (IL-1α), and tumor necrosis factor α (TNF-α), three cytokines necessary and sufficient to drive the formation of A1 astrocytes. Upregulation of these cytokines occurs first in CD11b + CD11c + cells followed by CD11b + CD11c − cells. Ablation of this pathway, by either genetic deletions of C1qa, IL-1α, and TNF-α, or treatment with glucagon-like peptide-1 receptor agonist NLY01, reduces A1 astrocyte transformation and RGC death. Together, these results highlight a neuroinflammatory mechanism of glaucomatous neurodegeneration that can be therapeutically targeted by NLY01 administration.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

GLP-1 Receptor Agonist NLY01 Reduces Retinal Inflammation and Neuron Death Secondary to Ocular Hypertension

et al. 2020

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“…ONH microglia and infiltrating monocytes express C3ar1 at high levels, while RGCs express C3ar1 at a lower level (Fig. 3d, [55,56]). Thus, C3ar1 deficiency in microglia and monocytes may affect their function or number in the ONH of ocular hypertensive eyes based on these expression data.…”

Section: Ocular Hypertension Affects C3ar1 Expression In the Optic Nementioning

confidence: 94%

Complement peptide C3a receptor 1 promotes optic nerve degeneration in DBA/2J mice

Harder

Williams

Braine

et al. 2020

J Neuroinflammation

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Background The risk of glaucoma increases significantly with age and exposure to elevated intraocular pressure, two factors linked with neuroinflammation. The complement cascade is a complex immune process with many bioactive end-products, including mediators of inflammation. Complement cascade activation has been shown in glaucoma patients and models of glaucoma. However, the function of complement-mediated inflammation in glaucoma is largely untested. Here, the complement peptide C3a receptor 1 was genetically disrupted in DBA/2J mice, an ocular hypertensive model of glaucoma, to test its contribution to neurodegeneration. Methods A null allele of C3ar1 was backcrossed into DBA/2J mice. Development of iris disease, ocular hypertension, optic nerve degeneration, retinal ganglion cell activity, loss of RGCs, and myeloid cell infiltration in C3ar1-deficient and sufficient DBA/2J mice were compared across multiple ages. RNA sequencing was performed on microglia from primary culture to determine global effects of C3ar1 on microglia gene expression. Results Deficiency in C3ar1 lowered the risk of degeneration in ocular hypertensive mice without affecting intraocular pressure elevation at 10.5 months of age. Differences were found in the percentage of mice affected, but not in individual characteristics of disease progression. The protective effect of C3ar1 deficiency was then overcome by additional aging and ocular hypertensive injury. Microglia and other myeloid-derived cells were the primary cells identified that express C3ar1. In the absence of C3ar1, microglial expression of genes associated with neuroinflammation and other immune functions were differentially expressed compared to WT. A network analysis of these data suggested that the IL10 signaling pathway is a major interaction partner of C3AR1 signaling in microglia. Conclusions C3AR1 was identified as a damaging neuroinflammatory factor. These data help suggest complement activation causes glaucomatous neurodegeneration through multiple mechanisms, including inflammation. Microglia and infiltrating myeloid cells expressed high levels of C3ar1 and are the primary candidates to mediate its effects. C3AR1 appeared to be a major regulator of microglia reactivity and neuroinflammatory function due to its interaction with IL10 signaling and other immune related pathways. Targeting myeloid-derived cells and C3AR1 signaling with therapies is expected to add to or improve neuroprotective therapeutic strategies.

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“…For example, in chronic hereditary glaucoma model DBA/2J mice, the aggregation, activation, and redistribution of microglia can be detected before RGC injury (Bosco et al, 2011). In DBA/2 J mice, the transcriptome of ONH microglia changes significantly in the metabolic, phagocytosis, inflammatory, and sensome pathways (Tribble et al, 2020). Among these, microglial surveillance and phagocytosis are downregulated, whereas metabolism-related transcripts are upregulated.…”

Section: Microglia In Glaucomamentioning

confidence: 99%

The Interaction Between Microglia and Macroglia in Glaucoma

et al. 2021

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Glaucoma, a neurodegenerative disease that leads to irreversible vision loss, is characterized by progressive loss of retinal ganglion cells (RGCs) and optic axons. To date, elevated intraocular pressure (IOP) has been recognized as the main phenotypic factor associated with glaucoma. However, some patients with normal IOP also have glaucomatous visual impairment and RGC loss. Unfortunately, the underlying mechanisms behind such cases remain unclear. Recent studies have suggested that retinal glia play significant roles in the initiation and progression of glaucoma. Multiple types of glial cells are activated in glaucoma. Microglia, for example, act as critical mediators that orchestrate the progression of neuroinflammation through pro-inflammatory cytokines. In contrast, macroglia (astrocytes and Müller cells) participate in retinal inflammatory responses as modulators and contribute to neuroprotection through the secretion of neurotrophic factors. Notably, research results have indicated that intricate interactions between microglia and macroglia might provide potential therapeutic targets for the prevention and treatment of glaucoma. In this review, we examine the specific roles of microglia and macroglia in open-angle glaucoma, including glaucoma in animal models, and analyze the interaction between these two cell types. In addition, we discuss potential treatment options based on the relationship between glial cells and neurons.

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Ocular hypertension suppresses homeostatic gene expression in optic nerve head microglia of DBA/2 J mice

Cited by 36 publications

References 84 publications

GLP-1 Receptor Agonist NLY01 Reduces Retinal Inflammation and Neuron Death Secondary to Ocular Hypertension

GLP-1 Receptor Agonist NLY01 Reduces Retinal Inflammation and Neuron Death Secondary to Ocular Hypertension

Complement peptide C3a receptor 1 promotes optic nerve degeneration in DBA/2J mice

The Interaction Between Microglia and Macroglia in Glaucoma

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