| Literature DB >> 33562488 |
Maria Jesus Rodrigo1,2,3, Amaya Pérez Del Palomar4,5, Alberto Montolío4,5, Silvia Mendez-Martinez1,2, Manuel Subias1,2, Maria Jose Cardiel6, Teresa Martinez-Rincon1,2, José Cegoñino4,5, José Maria Fraile7, Eugenio Vispe8, José Antonio Mayoral7, Vicente Polo1,2, Elena Garcia-Martin1,2,3.
Abstract
Intravitreal injection is the gold standard therapeutic option for posterior segment pathologies, and long-lasting release is necessary to avoid reinjections. There is no effective intravitreal treatment for glaucoma or other optic neuropathies in daily practice, nor is there a non-invasive method to monitor drug levels in the vitreous. Here we show that a glaucoma treatment combining a hypotensive and neuroprotective intravitreal formulation (IF) of brimonidine-Laponite (BRI/LAP) can be monitored non-invasively using vitreoretinal interface imaging captured with optical coherence tomography (OCT) over 24 weeks of follow-up. Qualitative and quantitative characterisation was achieved by analysing the changes in vitreous (VIT) signal intensity, expressed as a ratio of retinal pigment epithelium (RPE) intensity. Vitreous hyperreflective aggregates mixed in the vitreous and tended to settle on the retinal surface. Relative intensity and aggregate size progressively decreased over 24 weeks in treated rat eyes as the BRI/LAP IF degraded. VIT/RPE relative intensity and total aggregate area correlated with brimonidine levels measured in the eye. The OCT-derived VIT/RPE relative intensity may be a useful and objective marker for non-invasive monitoring of BRI/LAP IF.Entities:
Keywords: Laponite; brimonidine; drug delivery; glaucoma; intravitreal; monitoring; nanomedicine; optical coherence tomography; vitreous
Year: 2021 PMID: 33562488 PMCID: PMC7915309 DOI: 10.3390/pharmaceutics13020217
Source DB: PubMed Journal: Pharmaceutics ISSN: 1999-4923 Impact factor: 6.321