Could giant viruses be considered as a biotechnological tool for preventing and controlling Acanthamoeba infections?

The aim of the study was to evaluate the efficiency of mimivirus as a potential therapeutic and prophylactic tool against Acanthamoeba castellanii, the etiological agent of Acanthamoeba keratitis, a progressive corneal infection, which is commonly associated with the use of contact lenses and can le...

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Bibliographic Details
Published in:Journal of applied microbiology 2024-03, Vol.135 (3)
Main Authors: Crispim, Ana Paula Correia, Magalhães, Mateus Sá Serafim, Costa, Adriana Oliveira, Abrahão, Jônatas Santos
Format: Article
Language:English
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Summary:The aim of the study was to evaluate the efficiency of mimivirus as a potential therapeutic and prophylactic tool against Acanthamoeba castellanii, the etiological agent of Acanthamoeba keratitis, a progressive corneal infection, which is commonly associated with the use of contact lenses and can lead to blindness if not properly treated. mimivirus particles were tested in different multiplicity of infection, along with commercial multipurpose contact lenses' solutions, aiming to assess their ability to prevent encystment and excystment of A. castellanii. Solutions were evaluated for their amoebicidal potential and cytotoxicity in MDCK cells, as well as their effectiveness in preventing A. castellanii damage in MDCK cells. Results indicated that mimivirus was able to inhibit the formation of A. castellanii cysts, even in the presence of Neff encystment solution. Mimivirus also showed greater effectiveness in controlling A. castellanii excystment compared to commercial solutions. Additionally, mimivirus solution was more effective in preventing damage caused by A. castellanii, presented greater amoebicidal activity, and were less cytotoxic to MDCK cells than commercial MPS. mimivirus demonstrates a greater ability to inhibit A. castellanii encystment and excystment compared to commercial multipurpose contact lens solutions. Additionally, mimivirus is less toxic to MDCK cells than those commercial solutions. New studies utilizing in vivo models will be crucial for confirming safety and efficacy parameters.
ISSN:1365-2672
1365-2672
DOI:10.1093/jambio/lxae044