Comparison of Glaucoma-Relevant Transcriptomic Datasets Identifies Novel Drug Targets for Retinal Ganglion Cell Neuroprotection

Enz, Tim J; Tribble, James R.; Williams, Pete A.

doi:10.3390/jcm10173938

Cited by 9 publications

(9 citation statements)

References 40 publications

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“…The retinal explant model has previously been demonstrated to be a useful tool for the rapid exploration of neurodegenerative and neuroprotective mechanisms in mouse, rat, pig, and human retina ( Bull et al, 2011 ; Bell et al, 2016 ; Binley et al, 2016 ; Osborne et al, 2016 ; Williams et al, 2017a ; Tribble et al, 2021c ; Enz, Tribble and Williams, 2021 ). Our data demonstrate that it is also highly amenable in investigating neuroinflammation without the loss of spatial interaction that occurs in cell culture or direct insult to glial and astrocytes that may occur from cutting brain slices for culture (as, in this model, only retinal ganglion cell axons are axotomized).…”

Section: Discussionmentioning

confidence: 99%

“…In the CNS, VPA has demonstrated both neuroprotective and anti-inflammatory effects in diverse animal models of neurodegenerative conditions including spinal cord injury, traumatic brain injury, stroke, Parkinson’s disease, and optic neuritis ( Kim et al, 2007 ; Liu et al, 2017 ; Chen S et al, 2018 ; Chen X et al, 2018 ; Chang et al, 2019 ; Kim et al, 2019 ). Using a comparative transcriptomics approach, we recently identified VPA as a potential modifier of expression of genes common to retinal ganglion cell axon degeneration ( Enz, Tribble and Williams, 2021 ) (the susceptible neuron in many optic neuropathies including glaucoma, Leber’s hereditary optic neuropathy, and autosomal dominant optic atrophy). Pathway analysis of genes revealed neuroinflammatory signaling pathways to be the most commonly shared element and, as hypothesized, VPA provided significant neuroprotection to retinal ganglion cells post-axotomy.…”

Section: Introductionmentioning

confidence: 99%

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Valproic Acid Reduces Neuroinflammation to Provide Retinal Ganglion Cell Neuroprotection in the Retina Axotomy Model

Tribble

Kastanaki

Uslular

et al. 2022

Front. Cell Dev. Biol.

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Neuroinflammation is a critical and targetable pathogenic component of neurodegenerative diseases, including glaucoma, the leading cause of irreversible blindness. Valproic acid has previously been demonstrated to reduce neuroinflammation and is neuroprotective in a number of experimental settings. To determine whether valproic acid can limit retinal neuroinflammation and protect retinal neurons we used an ex vivo retina explant (axotomy) model to isolate resident glial responses from blood-derived monocytes. Neuroinflammatory status was defined using high resolution confocal imaging with 3D morphological reconstruction and cytokine protein arrays. Valproic acid significantly reduced microglia and astrocyte morphological changes, consistent with a reduction in pro-inflammatory phenotypes. Cytokine profiling demonstrated that valproic acid significantly attenuated or prevented expression of pro-inflammatory cytokines in injured retina. This identifies that the retinal explant model as a useful tool to explore resident neuroinflammation in a rapid timescale whilst maintaining a complex system of cell interactions and valproic acid as a useful drug to further explore anti-neuroinflammatory strategies in retinal disease.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Valproic Acid Reduces Neuroinflammation to Provide Retinal Ganglion Cell Neuroprotection in the Retina Axotomy Model

Tribble

Kastanaki

Uslular

et al. 2022

Front. Cell Dev. Biol.

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“…There are many other DEGs that we were unable to cover in the scope of this review but may ultimately play important roles in neuroprotection. Several key review articles have previously organized and described relevant genes and molecular mechanisms of neurodegeneration in glaucoma (142)(143)(144). Most recently, Wang et al (145) have also summarized commonly upregulated or downregulated genes by comparing transcriptomic data in several glaucoma mouse models and optic nerve crush models, most of which we have also included in this review.…”

Section: Concluding Marksmentioning

confidence: 99%

Differential Retinal Ganglion Cell Vulnerability, A Critical Clue for the Identification of Neuroprotective Genes in Glaucoma

Amin

Kuwajima²

2022

Front. Ophthalmol.

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Retinal ganglion cells (RGCs) are the neurons in the retina which directly project to the brain and transmit visual information along the optic nerve. Glaucoma, one of the leading causes of blindness, is characterized by elevated intraocular pressure (IOP) and degeneration of the optic nerve, which is followed by RGC death. Currently, there are no clinical therapeutic drugs or molecular interventions that prevent RGC death outside of IOP reduction. In order to overcome these major barriers, an increased number of studies have utilized the following combined analytical methods: well-established rodent models of glaucoma including optic nerve injury models and transcriptomic gene expression profiling, resulting in the successful identification of molecules and signaling pathways relevant to RGC protection. In this review, we present a comprehensive overview of pathological features in a variety of animal models of glaucoma and top differentially expressed genes (DEGs) depending on disease progression, RGC subtypes, retinal regions or animal species. By comparing top DEGs among those different transcriptome profiles, we discuss whether commonly listed DEGs could be defined as potential novel therapeutic targets in glaucoma, which will facilitate development of future therapeutic neuroprotective strategies for treatments of human patients in glaucoma.

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“…Moreover, regarding the cornea, the first large-scale single-cell dataset was just published ( Collin et al, 2021 ). Finally, a recent meta-analysis of glaucoma-related gene expression yielded drug candidates protecting retinal ganglion cells, as described by Enz et al (2021) .…”

Section: Introductionmentioning

confidence: 99%

Gene Expression Data for Investigating Glaucoma Treatment Options and Pharmacology in the Anterior Segment, State-of-the-Art and Future Directions

Fuellen

Jünemann

2022

Front. Neurosci.

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Glaucoma treatment options as well as its etiology are far from understood. Gene expression (transcriptomics) data of the anterior segment of the eye can help by elucidating the molecular-mechanistic underpinnings, and we present an up-to-date description and discussion of what gene expression data are publicly available, and for which purposes these can be used. We feature the few resources covering all segments of the eye, and we then specifically focus on the anterior segment, and provide an extensive list of the Gene Expression Omnibus data that may be useful. We also feature single-cell data of relevance, particularly three datasets from tissues of relevance to aqueous humor outflow. We describe how the data have been used by researchers, by following up resource citations and data re-analyses. We discuss datasets and analyses pertaining to fibrosis following glaucoma surgery, and to glaucoma resulting from the use of steroids. We conclude by pointing out the current lack and underutilization of ocular gene expression data, and how the state of the art is expected to improve in the future.

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Comparison of Glaucoma-Relevant Transcriptomic Datasets Identifies Novel Drug Targets for Retinal Ganglion Cell Neuroprotection

Cited by 9 publications

References 40 publications

Valproic Acid Reduces Neuroinflammation to Provide Retinal Ganglion Cell Neuroprotection in the Retina Axotomy Model

Valproic Acid Reduces Neuroinflammation to Provide Retinal Ganglion Cell Neuroprotection in the Retina Axotomy Model

Differential Retinal Ganglion Cell Vulnerability, A Critical Clue for the Identification of Neuroprotective Genes in Glaucoma

Gene Expression Data for Investigating Glaucoma Treatment Options and Pharmacology in the Anterior Segment, State-of-the-Art and Future Directions

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