Your search keyword '"Gore, Ariel"' showing total 3 results

1. Ocular surface histopathological insult following sarin and VX exposure and potential treatments in the rat model.

Author

Gore A, Lazar S, Yacov G, Gez R, Rabinowitz I, Nili U, Egoz I, and Kadar T

Subjects

Acetylcholinesterase metabolism, Animals, Cytoprotection, Dose-Response Relationship, Drug, Eye enzymology, Eye pathology, Eye physiopathology, GPI-Linked Proteins antagonists & inhibitors, GPI-Linked Proteins metabolism, Male, Miosis chemically induced, Miosis pathology, Miosis physiopathology, Rats, Long-Evans, Time Factors, Antidotes pharmacology, Blinking drug effects, Chemical Warfare Agents toxicity, Cholinesterase Inhibitors toxicity, Eye drug effects, Miosis prevention & control, Muscarinic Antagonists pharmacology, Organothiophosphorus Compounds toxicity, Sarin toxicity

Abstract

Eye exposure to organophosphate (OP) chemical warfare irreversible acetylcholinesterase inhibitors, results in long-term miosis and impaired visual function. In contrast to the well-documented miotic and ciliary muscle spasm observed following chemical warfare, OP ocular exposure, little is known regarding the ocular surface histopathological insult. The aim of the present study was to determine the degree of the ocular surface insult following sarin or VX ocular exposure and to evaluate potential anti-cholinergic treatments in counteracting this insult. Rats that were whole body exposed to various sarin concentrations (0.049-43 μg/L; 5 min exposure), showed a dose-dependent miotic response and light reflex impairment. Following whole body sarin exposure, a dose dependent ocular surface histopathological insult was developed. A week following exposure to a low concentration of 0.05 μg/L, conjunctival pathology was observed, while corneal insult was noticed only following exposure to a concentration of 0.5 μg/L and above. Both tissues presented poorer outcomes when exposed to higher sarin concentrations. In contrast, eyes topically exposed to 1 μg sarin demonstrated no ocular insult a week following exposure. On the contrary, topical exposure to 1 μg VX resulted in a significant corneal insult. Anticholinergic treatments such as 0.1% atropine or 2% homatropine, given shortly following VX exposure, counteracted this insult. The results of this study show that not only do anti-cholinergic treatments counteract the miotic response, but also prevent the histopathological insult observed when given shortly following OP exposure., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

2. Efficacy assessment of various anticholinergic agents against topical sarin-induced miosis and visual impairment in rats.

Author

Gore A, Brandeis R, Egoz I, Peri D, Turetz J, and Bloch-Shilderman E

Subjects

Animals, Male, Miosis physiopathology, Rats, Rats, Long-Evans, Vision Disorders physiopathology, Cholinesterase Inhibitors toxicity, Miosis chemically induced, Sarin toxicity, Vision Disorders chemically induced

Abstract

Eye exposure to the organophosphorus (OP) irreversible acetylcholinesterase inhibitor sarin results in long-term miosis and reduction in visual function. Anticholinergic drugs, such as atropine or homatropine, which are used topically in order to counter these effects may produce mydriasis and partial cycloplegia, which may worsen visual performance. This study was aimed to test the efficacy of short-acting anticholinergic drugs against sarin-induced miosis and visual impairment, which will minimally insult vision. Long-Evans rats, exposed topically to various sarin doses from 0 to 10 μg, showed a dose-dependent miosis, which returned to pre-exposure levels within 24-48 h. Tropicamide treatment rapidly widened the miotic effect to a different extent depending on time following treatment and dosage given. Cyclopentolate, however, showed a delayed response that finally widened the pupils in a dose-dependent manner. Atropine treatment showed a rapid widening of the pinpoint pupils exceeding baseline level finally causing mydriasis. Light reflex test showed that the contraction ability of the iris following atropine treatment was impaired, as opposed to the use of tropicamide which facilitated the iris contraction, similar to control. Finally, tropicamide and atropine treatments ameliorated the visual impairment, as opposed to cyclopentolate, which worsened visual performance. Considering that tropicamide treatment against sarin exposure did not cause mydriasis nor did it impair the iris contraction flexibility as a response to light, the use of this drug should be taken into consideration as a first-choice topical treatment against OP intoxication.

Published

2012

3. Optimization of the Ocular Treatment Following Organophosphate Nerve Agent Insult.

Author

Egoz, Inbal, Nili, Uri, Grauer, Ettie, and Gore, Ariel

Subjects

ACETYLCHOLINESTERASE genetics, PARASYMPATHOLYTIC agents, VISION disorders, MIOSIS, HOMATROPINE

Abstract

Eye exposure to organophosphate (OP) irreversible acetylcholinesterase inhibitors, results in long-term miosis and impaired visual function. The aim of this study was to find an anticholinergic antidote, which would counteract miosis and visual impairment induced by the nerve agents sarin and VX with minimal untoward side-effects. Rat pupil width and light reflex were evaluated from 15min up to 2 weeks following topical OP exposure with or without topical ocular treatment of atropine or homatropine or with a combined intramuscular treatment of trimedoxime (TMB-4) and atropine (TA). Visual function following insult and treatment was assessed using a cued Morris water maze task. Topical VX exposure showed a dose-dependent miosis with a significant reduction in visual function similar to the effect seen following sarin exposure. Homatropine (2%; w/v) and atropine (0.1%; w/v) treatment ameliorated both sarin and VX-induced miosis and the resulting visual impairment. TA treatment was sufficient in ameliorating the sarin-induced ocular impairment while an additional ocular treatment with either 0.1% atropine or 2% homatropine was necessary following VX exposure. To conclude the use of 0.1% atropine or 2% homatropine was beneficial in ameliorating the ocular insult following VX or sarin ocular exposure and thus should be considered as universal treatments against this intoxication. The findings also emphasize the necessity of additional ocular treatment to the systemic treatment in visually impaired casualties following VX exposure. [ABSTRACT FROM AUTHOR]

Published

2017