Evaluation of the neuroprotective efficacy of the gramine derivative ITH12657 against NMDA-induced excitotoxicity in the rat retina

FRONTIERS IN NEUROANATOMY(2024)

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摘要
Purpose: The aim of this study was to investigate, the neuroprotective effects of a new Gramine derivative named: ITH12657, in a model of retinal excitotoxicity induced by intravitreal injection of NMDA. Methods: Adult Sprague Dawley rats received an intravitreal injection of 100 mM NMDA in their left eye and were treated daily with subcutaneous injections of ITH12657 or vehicle. The best dose-response, therapeutic window study, and optimal treatment duration of ITH12657 were studied. Based on the best survival of Brn3a + RGCs obtained from the above-mentioned studies, the protective effects of ITH12657 were studied in vivo (retinal thickness and full-field Electroretinography), and ex vivo by quantifying the surviving population of Brn3a + RGCs, alpha RGCs and their subtypes alpha-ONsRGCs, alpha-ONtRGCs, and alpha-OFFRGCs. Results: Administration of 10 mg/kg ITH12657, starting 12 h before NMDA injection and dispensed for 3 days, resulted in the best significant protection of Brn3a + RGCs against NMDA-induced excitotoxicity. In vivo, ITH12657-treated rats showed significant preservation of retinal thickness and functional protection against NMDA-induced retinal excitotoxicity. Ex vivo results showed that ITH12657 afforded a significant protection against NMDA-induced excitotoxicity for the populations of Brn3a + RGC, alpha RGC, and alpha ONs-RGC, but not for the population of alpha OFF-RGC, while the population of alpha-ONtRGC was fully resistant to NMDA-induced excitotoxicity. Conclusion: Subcutaneous administration of ITH12657 at 10 mg/kg, initiated 12 h before NMDA-induced retinal injury and continued for 3 days, resulted in the best protection of Brn3a + RGCs, alpha RGC, and alpha ONs-RGC against excitotoxicity-induced RGC death. The population of alpha OFF-RGCs was extremely sensitive while alpha-ONtRGCs were fully resistant to NMDA-induced excitotoxicity.
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NMDA excitotoxicity,glaucoma,retina ganglion cell,neuroprotection,Brn3a+RGCs,SD-OCT,alpha RGCs,retina calcium blocker
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