Molecular imaging of retinal endothelial injury in diabetic animals

Message:
Abstract:
Purpose
Diabetic retinopathy is a leading cause of vision loss. There is a great need for early diagnosis prior to the occurrence of irreversible structural damages. Expression of endothelial adhesion molecules is observed before the onset of diabetic vascular damage; however, to date, these molecules cannot be visualized in vivo.
Methods
To quantify the expression of endothelial surface molecules, we generated imaging probes that bind to ICAM‑1. The α‑ICAM‑1 probes were characterized via flow cytometry under microfluidic conditions. Probes were systemically injected into normal and diabetic rats, and their adhesion in the retinal microvessels was visualized via confocal scanning laser ophthalmoscopy. Histology was performed to validate in vivo imaging results. Vascular pathologies were visualized using trypsin‑digested retinal preparations.
Results
The α‑ICAM‑1 probes showed significantly higher adhesion to retinal microvessels in diabetic rats than in normal controls (P
Conclusion
Results indicate that molecular imaging can be used to detect subtle changes in the diabetic retina prior to the occurrence of irreversible pathology. Thus, ICAM‑1 could serve as a diagnostic target in patients with diabetes. This study provides a proof of principle for non‑invasive subclinical diagnosis in experimental diabetic retinopathy. Further development of this technology could improve management of diabetic complications.
Language:
English
Published:
Journal of Ophthalmic and Vision Research, Volume:12 Issue: 2, Apr-Jun 2017
Page:
175
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