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Targeting the tight junction protein, zonula occludens-1, with the connexin43 mimetic peptide, αCT1, reduces VEGF-dependent RPE pathophysiology
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نویسنده
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Obert Elisabeth ,Strauss Randy ,Brandon Carlene ,Grek Christina ,Ghatnekar Gautam ,Gourdie Robert ,Rohrer Bärbel
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منبع
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journal of molecular medicine - 2017 - دوره : 95 - شماره : 5 - صفحه:535 -552
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چکیده
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A critical target tissue in age-related macular degeneration (amd) is the retinal pigment epithelium (rpe), which forms the outer blood-retina barrier (brb). rpe-barrier dysfunction might result from attenuation/disruption of intercellular tight junctions. zonula occludens-1 (zo-1) is a major structural protein of intercellular junctions. a connexin43-based peptide mimetic, αct1, was developed to competitively block interactions at the pdz2 domain of zo-1, thereby inhibiting ligands that selectively bind to this domain. we hypothesized that targeting zo-1 signaling using αct1 would maintain brb integrity and reduce rpe pathophysiology by stabilizing gap- and/or tight-junctions. rpe-cell barrier dysfunction was generated in mice using laser photocoagulation triggering choroidal neovascularization (cnv) or bright light exposure leading to morphological damage. αct1 was delivered via eye drops. αct1 treatment reduced cnv development and fluid leakage as determined by optical coherence tomography, and damage was correlated with disruption in cellular integrity of surrounding rpe cells. light damage significantly disrupted rpe cell morphology as determined by zo-1 and occludin staining and tiling pattern analysis, which was prevented by αct1 pre-treatment. in vitro experiments using rpe and mdck monolayers indicated that αct1 stabilizes tight junctions, independent of its effects on cx43. taken together, stabilization of intercellular junctions by αct1 was effective in ameliorating rpe dysfunction in models of amd-like pathology.
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کلیدواژه
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Retinal pigment epithelium ,Connexin43 ,Tight junctions ,Choroidal neovascularization ,Light damage ,Vascular endothelial growth factor ,Age-related macular degeneration
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آدرس
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Medical University of South Carolina, Department of Neuroscience, USA, Virginia Tech Carilion Research Institute, USA, Medical University of South Carolina, Department of Ophthalmology, USA, FirstString Research Inc., USA, FirstString Research Inc., USA, Virginia Tech Carilion Research Institute, USA, Medical University of South Carolina, Department of Neuroscience, Department of Ophthalmology, USA. Ralph H. Johnson VA Medical Center, USA
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Authors
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