Abstract
Diabetic retinopathy (DR) is the most common microvascular complication of diabetes and one of the major causes of blindness worldwide. The pathogenesis of DR has been investigated using several animal models of diabetes. These models have been generated by pharmacological induction, feeding a galactose diet, and spontaneously by selective inbreeding or genetic modification. Among the available animal models, rodents have been studied most extensively owing to their short generation time and the inherited hyperglycemia and/or obesity that affect certain strains. In particular, mice have proven useful for studying DR and evaluating novel therapies because of their amenability to genetic manipulation. Mouse models suitable for replicating the early, non-proliferative stages of the retinopathy have been characterized, but no animal model has yet been found to demonstrate all of the vascular and neural complications that are associated with the advanced, proliferative stages of DR that occur in humans. In this review, we summarize commonly used animal models of DR, and briefly outline the in vivo imaging techniques used for characterization of DR in these models. Through highlighting the ocular pathological findings, clinical implications, advantages and disadvantages of these models, we provide essential information for planning experimental studies of DR that will lead to new strategies for its prevention and treatment.
Highlights
Diabetic retinopathy (DR), a major complication of diabetes mellitus, is one of the leading causes of blindness worldwide
Treatment of DR can only be achieved through an enhanced understanding of disease pathogenesis; because most structural, functional and biochemical studies cannot be carried out in human subjects, animal models are essential for studying DR pathology, and for developing new and better treatments
DR can be classified into non-proliferative DR (NPDR) and proliferative DR (PDR) (Cheung et al, 2010)
Summary
Diabetic retinopathy (DR), a major complication of diabetes mellitus, is one of the leading causes of blindness worldwide. An insight into the retinal vessel caliber changes in animal models of DR could potentially help to characterize the structure and pathology of the microcirculation, and to examine its relationship to systemic vascular diseases in diabetes. STZ-induced diabetic B6 mice demonstrated acellular capillaries, apoptosis of vascular cells and pericyte ghosts in the retina, the hallmark of early characteristics of DR (Feit-Leichman et al, 2005), at ~6 months after the onset of diabetes.
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