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Diabetic retinopathy and diabetic macular edema: pathophysiology, screening, and novel therapies.

机译:糖尿病性视网膜病变和糖尿病性黄斑水肿:病理生理学,筛查和新疗法。

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摘要

Diabetic retinopathy (DR) and diabetic macular edema (DME) are leading causes of blindness in the working-age population of most developed countries. The increasing number of individuals with diabetes worldwide suggests that DR and DME will continue to be major contributors to vision loss and associated functional impairment for years to come. Early detection of retinopathy in individuals with diabetes is critical in preventing visual loss, but current methods of screening fail to identify a sizable number of high-risk patients. The control of diabetes-associated metabolic abnormalities (i.e., hyperglycemia, hyperlipidemia, and hypertension) is also important in preserving visual function because these conditions have been identified as risk factors for both the development and progression of DR/DME. The currently available interventions for DR/DME, laser photocoagulation and vitrectomy, only target advanced stages of disease. Several biochemical mechanisms, including protein kinase C-beta activation, increased vascular endothelial growth factor production, oxidative stress, and accumulation of intracellular sorbitol and advanced glycosylation end products, may contribute to the vascular disruptions that characterize DR/DME. The inhibition of these pathways holds the promise of intervention for DR at earlier non-sight-threatening stages. To implement new therapies effectively, more individuals will need to be screened for DR/DME at earlier stages-a process requiring both improved technology and interdisciplinary cooperation among physicians caring for patients with diabetes.
机译:糖尿病性视网膜病(DR)和糖尿病性黄斑水肿(DME)是大多数发达国家劳动年龄人群致盲的主要原因。在世界范围内,越来越多的糖尿病患者表明DR和DME在未来几年将继续成为视力丧失和相关功能障碍的主要贡献者。在糖尿病患者中及早发现视网膜病变对于预防视力丧失至关重要,但是目前的筛查方法无法识别出大量的高危患者。糖尿病相关的代谢异常(即高血糖,高血脂和高血压)的控制对于维持视觉功能也很重要,因为这些条件已被确定为DR / DME发生和发展的危险因素。 DR / DME,激光光凝和玻璃体切除术的当前可用干预措施仅针对疾病的晚期阶段。几种生物化学机制,包括蛋白激酶C-β活化,增加的血管内皮生长因子产生,氧化应激以及细胞内山梨糖醇和高级糖基化终产物的积累,可能会导致表征DR / DME的血管破裂。这些途径的抑制有望在较早的非视力威胁阶段干预DR。为了有效地实施新疗法,将需要在早期对更多的患者进行DR / DME筛查-这一过程既需要技术改进,又需要在照顾糖尿病患者的医师之间开展跨学科合作。

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