首页> 外文期刊>Journal of ocular pharmacology and therapeutics: The official journal of the Association for Ocular Pharmacology and Therapeutics >Evaluation of the vascular targeting agent combretastatin a-4 prodrug on retinal neovascularization in the galactose-fed dog.
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Evaluation of the vascular targeting agent combretastatin a-4 prodrug on retinal neovascularization in the galactose-fed dog.

机译:在半乳糖喂养的狗中评估血管靶向剂康维他汀a-4前体药物对视网膜新血管形成的作用。

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PURPOSE: Combretastatin A-4 (CA-4) is a vascular targeting agent known to rapidly shut off blood flow in new vessels and, as a result, regress neovascularization. In this pilot study, the ability of CA-4 to modify retinal neovascularization, which results in altered retinal vessel blood flow and retinal permeability, was evaluated in aphakic long-term galactose-fed beagles, an animal model that develops diabetes-like retinal neovascularization. METHODS: Two (2) groups of aphakic dogs, each group comprised of 4 galactose-fed dogs and 2 age-matched controls dogs, were utilized. Each group initially received the combretastatin A-4-phosphate prodrug (CA-4P) as either sub-Tenon's injections, administered at the corneoscleral junction, or intravitreal injections. Six (6) weeks after this treatment, all dogs also received systemic (intravenous) injections of CA-4P. Retinal vascular changes were monitored at 2-week intervals by fluorescein angiography. RESULTS: All galactose-fed dogs demonstrated the presence of retinal neovascular lesions by fluorescein angiograms. Fluorescein leakage or perfusion through neovascular vessels was not altered by either sub-Tenon's, intravitreal, or systemic CA-4P administration. Whereas CA-4P was well tolerated by the healthy eyes of the control animals, its administration to some galactose-fed dogs was associated with corneal edema and increases in intraocular pressure following sub-Tenon's and intraocular injections. CONCLUSIONS: Neovascularization in the galactose-fed dog progresses over a period of years, similar to that observed with clinical diabetic retinopathy. The failure of CA-4P to ameliorate neovascularization suggests that chronic, long-term administration may be required to destroy the slowly growing retinal endothelial cells.
机译:用途:Combretastatin A-4(CA-4)是一种血管靶向剂,已知可以迅速切断新血管中的血流,从而使新血管形成退行。在这项先导研究中,在无晶状体长期半乳糖喂养的小猎犬(一种发展为糖尿病样视网膜新血管形成的动物模型)中评估了CA-4修饰视网膜新血管形成的能力,从而导致视网膜血管血流和视网膜通透性的改变。 。方法:使用两(2)组无晶状犬,每组由4只半乳糖喂养的犬和2只年龄匹配的对照犬组成。每个组最初都接受康维他汀A-4-磷酸酯前药(CA-4P),作为蒂农子下注射,角膜巩膜交界处注射或玻璃体内注射。治疗后六(6)周,所有的狗也都接受了CA-4P的全身(静脉内)注射。通过荧光素血管造影术每两周监测一次视网膜血管的变化。结果:所有半乳糖喂养的狗通过荧光素血管造影显示视网膜新生血管病变的存在。蒂农氏,玻璃体内或全身CA-4P的施用不会改变荧光素通过新血管的渗漏或灌注。对照动物的健康眼睛对CA-4P有很好的耐受性,但对某些半乳糖喂养的狗施用CA-4P会导致角膜浮肿,并在特农氏和眼内注射后增加眼内压。结论:半乳糖喂养的狗的新生血管形成历时数年,与临床糖尿病性视网膜病变观察到的相似。 CA-4P未能改善新血管形成,提示可能需要长期长期给药才能破坏缓慢生长的视网膜内皮细胞。

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