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Literature DB >> 15985430

Involvement of inflammation, degradation, and apoptosis in a mouse model of glaucoma.

Xiaohong Zhou¹, Feng Li, Li Kong, Hiroshi Tomita, Chao Li, Wei Cao.

Abstract

Glaucoma is a common cause of blindness affecting at least 66 million people worldwide. Pigmentary glaucoma is one of the most common forms of secondary glaucoma, and its pathogenesis remains unclear. Interleukin-18 (IL-18) is an important regulator of innate and acquired immune responses and plays an important role in inflammatory/autoimmunity diseases. Using the DBA/2J mouse as an animal model of human pigmentary glaucoma, we demonstrated for the first time that the expression of the IL-18 protein and gene in the iris/ciliary body and level of IL-18 protein in the aqueous humor of DBA/2J mice are dramatically increased with age. This increase precedes the onset of clinical evidence of pigmentary glaucoma, implying a pathogenic role of inflammation/immunity in this disease. We also observed that activated NF-kappaB and phosphorylated MAPK are increased in the iris/ciliary body of DBA/2J mice, suggesting that both signaling pathways may be involved in IL-18 mediated pathogenesis of pigmentary glaucoma in the eyes of DBA/2J mice. In addition, matrix metalloproteinase-2 (MMP-2) expression in the iris/ciliary body and the activity of MMP-2 in the aqueous humor are increased whereas tissue inhibitor of matrix metalloproteinase-1 (TIMP-1) expression in the iris/ciliary body is decreased, indicating that the degradation process is involved in this mouse model of pigmentary glaucoma. Furthermore, the expressions of apoptosis-related genes, caspase-8, Fas, FADD, FAP, and FAF, and the activity of caspase-3 are increased in the iris/ciliary body of DBA/2J mice. Elucidation of biochemical and molecular mechanisms of IL-18 participation in the pathogenesis of pigmentary glaucoma should provide approaches for developing improved and targeted treatments to ameliorate this blinding disease. The possibility that altered IL-18 expression in the eye of DBA/2J mice initiates and/or amplifies the pathogenesis of pigmentary glaucoma requires further investigation.

Entities: Disease Gene Species

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Year: 2005 PMID： 15985430 DOI： 10.1074/jbc.M502641200

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

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Cited

64 in total

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Journal: Eye (Lond) Date: 2018-12-18 Impact factor: 3.775

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4. Western blot patterns of serum autoantibodies against optic nerve antigens in dogs with goniodysgenesis-related glaucoma.

Authors: Stephanie A Pumphrey; Stefano Pizzirani; Christopher G Pirie; M Sawkat Anwer; Tanya Logvinenko
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5. Early Involvement of Immune/Inflammatory Response Genes in Retinal Degeneration in DBA/2J Mice.

Authors: W Fan; X Li; W Wang; J S Mo; H Kaplan; N G F Cooper
Journal: Ophthalmol Eye Dis Date: 2010-03-11

6. Failure of axonal transport induces a spatially coincident increase in astrocyte BDNF prior to synapse loss in a central target.

Authors: S D Crish; J D Dapper; S E MacNamee; P Balaram; T N Sidorova; W S Lambert; D J Calkins
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Involvement of inflammation, degradation, and apoptosis in a mouse model of glaucoma.

1. Neuroprotective effect of overexpression of thioredoxin on photoreceptor degeneration in Tubby mice.

2. Kaempferol attenuates retinal ganglion cell death by suppressing NLRP1/NLRP3 inflammasomes and caspase-8 via JNK and NF-κB pathways in acute glaucoma.

3. Multiplex cytokine analysis reveals elevated concentration of interleukin-8 in glaucomatous aqueous humor.

4. Western blot patterns of serum autoantibodies against optic nerve antigens in dogs with goniodysgenesis-related glaucoma.

5. Early Involvement of Immune/Inflammatory Response Genes in Retinal Degeneration in DBA/2J Mice.

6. Failure of axonal transport induces a spatially coincident increase in astrocyte BDNF prior to synapse loss in a central target.

7. Gene and protein expression pilot profiling and biomarkers in an experimental mouse model of hypertensive glaucoma.

8. Longitudinal evaluation of retinal ganglion cell function and IOP in the DBA/2J mouse model of glaucoma.

9. IOP-dependent retinal ganglion cell dysfunction in glaucomatous DBA/2J mice.

10. Smoking, an additional risk factor in elder women with primary open-angle glaucoma.