Complement C3-targeted gene therapy restricts onset and progression of neurodegeneration in chronic mouse glaucoma

Bosco, Alejandra; Anderson, Sarah; Breen, Kevin T.; Romero, Carmelo García; Steele, Matt; Chiodo, Vince A.; Boye, Sanford L.; Hauswirth, William W.; Tomlinson, Stephen; Vetter, Monica L.

doi:10.1101/369181

Cited by 8 publications

(11 citation statements)

References 98 publications

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“…C1q is localized to RGC compartments (Stevens et al, ), and KO in the DBA/2J mouse is neuroprotective (Howell et al, ), while paradoxically KO of C3 worsens pathology (Harder et al, ), suggesting that the roles of complement are complex. Targeted inhibition of the C3 activation step by retinal gene therapy restricts the progression of neurodegeneration (Bosco et al ). AMD is associated with mutations in several complement proteins and the pathogenic role of complement system has received great attention (Anderson et al, ; Warwick et al, ; Bora et al, ; McHarg et al, ).…”

Section: Shared Pathways Of Microglia In Developmental and Disease Stmentioning

confidence: 99%

Developmental roles of microglia: A window into mechanisms of disease

Anderson

Vetter

2018

Developmental Dynamics

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Microglia are engineers of the CNS both in health and disease. In addition to the canonical immunological roles of clearing damaging entities and limiting the spread of toxicity and death, microglia remodel the CNS throughout life. While they have been extensively studied in disease and injury, due to their highly variable functions, their precise role in these contexts still remains uncertain. Over the last decade we have greatly expanded our understanding of microglial function, including their essential homeostatic roles during development. Here, we review these developmental roles, identify parallels in disease, and speculate whether developmental mechanisms reemerge in disease and injury.

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Section: Shared Pathways Of Microglia In Developmental and Disease Stmentioning

confidence: 99%

Developmental roles of microglia: A window into mechanisms of disease

Anderson

Vetter

2018

Developmental Dynamics

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“…Notably these data pointed to major neuroinflammatory changes at a pre-degenerative stage of disease, including changes in the complement system, endothelin system, and cell-adhesion pathways. Our group and others have experimentally validated molecules in these pathways to demonstrate their importance and role in glaucoma (from mouse to human [2,12,[23][24][25][26][27][28][29];). In addition, these pathways have been independently identified in other models of glaucomatous insult and retinal ganglion cell death (ocular hypertension, optic nerve crush, optic nerve transection / axotomy [30][31][32]) supporting the utility of DBA/2 J retina and optic nerve head tissue for modelling glaucoma.…”

Section: Introductionmentioning

confidence: 99%

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

et al. 2020

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Glaucoma is the leading cause of irreversible vision loss. Ocular hypertension is a major risk factor for glaucoma and recent work has demonstrated critical early neuroinflammatory insults occur in the optic nerve head following ocular hypertension. Microglia and infiltrating monocytes are likely candidates to drive these neuroinflammatory insults. However, the exact molecular identity / transcriptomic profile of microglia following ocular hypertensive insults is unknown. To elucidate the molecular identity of microglia after long-term exposure to ocular hypertension, we used a mouse model of glaucoma (DBA/2 J). We performed RNA-sequencing of microglia mRNA from the optic nerve head at a time point following ocular hypertensive insults, but preceding detectable neurodegeneration (with microglia identified as being CD45 lo /CD11b + /CD11c −). Furthermore, RNA-sequencing was performed on optic nerve head microglia from mice treated with radiation therapy, a potent therapy preventing neuroinflammatory insults. Transcriptomic profiling of optic nerve head microglia mRNA identifies metabolic priming with marked changes in mitochondrial gene expression, and changes to phagocytosis, inflammatory, and sensome pathways. The data predict that many functions of microglia that help maintain tissue homeostasis are affected. Comparative analysis of these data with data from previously published whole optic nerve head tissue or monocyte-only samples from DBA/2 J mice demonstrate that many of the neuroinflammatory signatures in these data sets arise from infiltrating monocytes and not reactive microglia. Finally, our data demonstrate that prophylactic radiation therapy of DBA/2 J mice potently abolishes these microglia metabolic transcriptomic changes at the same time points. Together, our data provide a unique resource for the community to help drive further hypothesis generation and testing in glaucoma.

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“…A1 astrocytes upregulate C3 , and C3 inhibitors were shown to reduce RGC cell death in the DBA/2J mouse model of glaucoma (Bosco et al, 2018). We demonstrate elevated C3 production following A1 activation and decreased C3 production following NLY01 inhibition in our glaucoma model.…”

Section: Cell Reportsmentioning

confidence: 48%

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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Complement C3-targeted gene therapy restricts onset and progression of neurodegeneration in chronic mouse glaucoma

Cited by 8 publications

References 98 publications

Developmental roles of microglia: A window into mechanisms of disease

Developmental roles of microglia: A window into mechanisms of disease

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

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

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