AI Article Synopsis
- The inflammatory response from oxidative stress is a key factor in dry eye disease, but just targeting oxygen-free radicals hasn't proven very effective in treatment.
- The unique structure of the eye makes it hard for drugs to work in high enough concentrations without causing side effects, creating a major challenge for effective therapy.
- An innovative approach using NLRP3 inhibitors encapsulated in polydopamine-based microgels shows promise for better treatment by improving drug delivery, enhancing effectiveness, and reducing potential side effects.
Article Abstract
The inflammatory response mediated by oxidative stress is the main pathogenesis of dry eye, but clinical observations have shown that scavenging oxygen-free radicals alone has limited therapeutic effect. Moreover, the unique anatomy and physiology of the ocular surface result in low bioavailability of drugs, and higher concentration is required to achieve the desired efficacy, which, however, may bring systemic side effects. These problems pose a challenge, but the revelation of the ROS-NLRP3-IL-1β signaling axis opens up new possibilities. In this investigation, an NLRP3 inhibitor was successfully encapsulated in polydopamine-based microgels and used for dry eye treatment. It was demonstrated that the well-designed microgels exhibited good biocompatibility, prolonged drug retention time on the ocular surface, and effective inhibition of corneal epithelial damage and cell apoptosis. In addition, due to the synergistic effect, the NLRP3 inhibitor-loaded microgels could exert enhanced oxygen radical scavenging and inflammation-inhibiting effects at a lower dose than monotherapy. These findings suggest that polydopamine-based microgels have advantages as ocular surface drug delivery platforms and have promising applications in oxidative damage-related inflammatory diseases in synergy with anti-inflammatory drugs.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9198461 | PMC |
| http://dx.doi.org/10.3389/fbioe.2022.913648 | DOI Listing |
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