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Vascular endothelial growth factor and ocular neovascularization.

机译:血管内皮生长因子和眼新血管形成。

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摘要

Okamoto et al have developed an extremely useful and interesting model of retinal and subretinal neovascularization. Using molecular techniques, they have developed a transgenic model driven by overexpression of VEGF, a growth factor demonstrated to play an important role in neovascularization in many ocular diseases. They have been able to demonstrate that VEGF overexpression is sufficient to cause intraretinal and subretinal neovascularization. The mouse model is relatively cheap and reliable, does not require any exogenous agent, and has many characteristics of clinical intraocular neovascularization. The new vessels develop in the outer retina and subretinal space and have a characteristic histological appearance. They leak fluorescein on angiography, demonstrating their similarity to human disease and allowing identification and grading of neovascularization in vivo. The model can be used to investigate molecular mechanisms of VEGF-dependent neovascularization, with applications beyond ocular eye disease. The model can also be used to study anti-angiogenic agents that have the potential to treat common blinding diseases such as age-related macular degeneration. Okamoto et al have made a substantial contribution to the angiogenesis field with this work, and one looks forward to future investigations.
机译:冈本等人开发了一种非常有用和有趣的视网膜和视网膜下新血管形成模型。他们使用分子技术开发了一种由VEGF过表达驱动的转基因模型,VEGF是一种生长因子,在许多眼部疾病的新生血管形成中被证明具有重要作用。他们已经能够证明VEGF过表达足以引起视网膜内和视网膜下新血管形成。小鼠模型相对便宜且可靠,不需要任何外源性试剂,并且具有临床眼内新血管形成的许多特征。新血管在视网膜外和视网膜下间隙发育,并具有特征性的组织学外观。他们在血管造影术上泄漏了荧光素,证明了它们与人类疾病的相似性,并允许体内新血管形成的鉴定和分级。该模型可用于研究VEGF依赖性新血管形成的分子机制,其应用范围不仅限于眼部疾病。该模型还可以用于研究具有治疗常见致盲性疾病(例如年龄相关性黄斑变性)潜力的抗血管生成药物。冈本等人的这项工作为血管生成领域做出了重大贡献,并期待着将来的研究。

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