Classical and Innovative Evidence for Therapeutic Strategies in Retinal Dysfunctions

Author:

Caruso Lorenzo1ORCID,Fields Matteo2ORCID,Rimondi Erika3ORCID,Zauli Giorgio4ORCID,Longo Giovanna2ORCID,Marcuzzi Annalisa2ORCID,Previati Maurizio2,Gonelli Arianna1,Zauli Enrico2,Milani Daniela2ORCID

Affiliation:

1. Department of Environmental and Prevention Sciences, University of Ferrara, 44121 Ferrara, Italy

2. Department of Translational Medicine, University of Ferrara, 44121 Ferrara, Italy

3. Department of Translational Medicine and LTTA Centre, University of Ferrara, 44121 Ferrara, Italy

4. Research Department, King Khaled Eye Specialist Hospital, Riyadh 11462, Saudi Arabia

Abstract

The human retina is a complex anatomical structure that has no regenerative capacity. The pathogenesis of most retinopathies can be attributed to inflammation, with the activation of the inflammasome protein platform, and to the impact of oxidative stress on the regulation of apoptosis and autophagy/mitophagy in retinal cells. In recent years, new therapeutic approaches to treat retinopathies have been investigated. Experimental data suggest that the secretome of mesenchymal cells could reduce oxidative stress, autophagy, and the apoptosis of retinal cells, and in turn, the secretome of the latter could induce changes in mesenchymal cells. Other studies have evidenced that noncoding (nc)RNAs might be new targets for retinopathy treatment and novel disease biomarkers since a correlation has been found between ncRNA levels and retinopathies. A new field to explore is the interaction observed between the ocular and intestinal microbiota; indeed, recent findings have shown that the alteration of gut microbiota seems to be linked to ocular diseases, suggesting a gut–eye axis. To explore new therapeutical strategies for retinopathies, it is important to use proper models that can mimic the complexity of the retina. In this context, retinal organoids represent a good model for the study of the pathophysiology of the retina.

Publisher

MDPI AG

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