Direct Detection of Reactive Nitrogen Species in Experimental Autoimmune Uveitis

Overview

Journal Korean J Ophthalmol

Specialty Ophthalmology

Date 2007 Apr 27

PMID 17460428

Authors

Sun Ryang Bae

Guey Shuang Wu

Alex Sevanian

Brian E Schultz

Ehud Zamir

Narsing A Rao

Affiliations

Soon will be listed here.

Abstract

Purpose: Demonstrate unequivocally the generation of nitric oxide in experimental autoimmune uveoretinitis by electron spin resonance spectroscopy (ESR) using ferrous iron complex of N-methyl-D-glucamine dithiocarbamate, (MGD)(2)-Fe(2+), as a spin trap.

Methods: Experimental autoimmune uveitis was induced in Lewis rats, and at the peak of the intraocular inflammation, the animals received intravitreous injections of the spin trap. The retina and choroid dissected from the enucleated globes were subjected to ESR. Similarly, the retina and choroid obtained at the peak of experimental autoimmune uveo-retinitis (EAU) were placed in a vial containing luminal, and chemiluminescence was counted on a Packard liquid scintillation analyzer.

Results: The ESR three-line spectrum (g=2.04; a(N)=12.5 G) obtained was characteristic of the adduct [(MGD)(2)-Fe(2+)-NO]. The majority of this signal was eliminated by the inducible nitric oxide synthase (iNOS) specific inhibitor aminoguanidine injected inflamed retina was detected when compared with that of the non inflamed controls. The chemiluminescent activity was further increased two-fold by the addition of bicarbonate to the inflamed retina; the phenomenon is attributable only to the presence of a high steady-state concentration of peroxynitrite.

Conclusions: The study shows an unequivocal presence of nitric oxide in EAU retina and choroid and the generation of peroxynitrite. High levels of these reactive nitrogen species generated in the inflamed retina and choroids are certain to cause irreversible tissue damage, especially at the susceptible sites such as photoreceptors.

Citing Articles

Nitric oxide potentiates TNF-α-induced neurotoxicity through suppression of NF-κB.

Nakaizumi A, Horie T, Kida T, Kurimoto T, Sugiyama T, Ikeda T Cell Mol Neurobiol. 2011; 32(1):95-106.

PMID: 21833550 PMC: 11498544. DOI: 10.1007/s10571-011-9739-5.

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