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Invest Ophthalmol Vis SciAugust 20109 citations

Experimental intracameral injection of vancomycin microparticles in rabbits.

Kodjikian Laurent, Couprie Jérémy, Hachicha Walid, Timour Quadiri, Devouassoux Mojgan, Builles Nicolas, Hartmann Daniel, Fessi Hatem


AI Summary

Vancomycin microparticles effectively prevented experimental endophthalmitis in rabbits, releasing drug for hours with only transient, mild retinal inflammation, suggesting potential for cataract surgery prophylaxis.

Abstract

Purpose

To evaluate the in vivo toxicity and efficacy of previously developed poly-(lactide-co-glycolide)-vancomycin-based microparticles (V-MPLs) for eventual use for endophthalmitis prophylaxis during cataract surgery.

Methods

The intraocular vancomycin concentration profile was evaluated after V-MPL injection into the anterior chamber of rabbit eyes. The toxicology of V-MPLs versus MPLs alone was tested by corneal cellular counting and retinal histology. The prophylactic efficacy of the V-MPLs was evaluated by bacterial counts after introducing contaminated intraocular lenses (IOLs) together with the V-MPLs into one anterior chamber of phakic rabbit eyes or without V-MPLs in control rabbit eyes.

Results

Intraocular V-MPLs produced effective vancomycin concentrations over at least 6 hours. Corneal counts revealed no significant increase in dead cells. Retinal toxicity manifested as inflammation 3 hours after injection, reaching its maximum between 12 hours and 24 hours, decreasing by 48 hours, and completely disappearing at 72 hours. Inflammation was similar between V-MPLs and MPLs. Untreated eyes implanted with highly infected IOLs showed severe, reproducible endophthalmitis. No sign of infection was observed with infected IOLs and concomitant V-MPL treatment, supported by bacterial counts showing a significant decrease in colony-forming Staphylococcus epidermidis units in the anterior chamber and on the implant surfaces within 6 hours.

Conclusions

The present study demonstrated the release and toxicologic properties of the authors' newly developed V-MPLs in vivo. In addition, the rabbit model shows that V-MPLs are effective in reducing the risk of experimental endophthalmitis.


MeSH Terms

AnimalsAnterior ChamberAnti-Bacterial AgentsAqueous HumorBiological AvailabilityCell CountChromatography, High Pressure LiquidColony Count, MicrobialDisease Models, AnimalEndophthalmitisEndothelium, CornealEye Infections, BacterialHalf-LifeInjectionsIrisLens Implantation, IntraocularLenses, IntraocularMaleParticle SizePolyglactin 910RabbitsRetinaStaphylococcal InfectionsStaphylococcus epidermidisVancomycin

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