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首页> 外文期刊>Retina >Effect of squalamine on iris neovascularization in monkeys.
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Effect of squalamine on iris neovascularization in monkeys.

机译:角鲨胺对猴子虹膜新生血管的影响。

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PURPOSE: To investigate the effect of squalamine, an antiangiogenic aminosterol, in an experimental model of iris neovascularization. METHODS: Iris neovascularization was created in cynomolgus monkeys by occluding retinal veins with an argon laser and inducing persistent hypotony with a central corneal suture. Twenty-four eyes were treated in three groups. In Group 1, four eyes were injected intravitreally with 3 microg/0.1 mL squalamine and four eyes with balanced saline solution (controls) immediately after vein occlusion (day 1); injections were repeated every 3 days for 3 weeks. In Group 2, 1 mg/kg squalamine was administered with intravenous infusion in dextrose 5% in four animals; four control animals received only dextrose. Infusions began on day 1 and were repeated every 3 days for 3 weeks. In Group 3, after development of iris neovascularization on day 7, 1 mg/kg squalamine was injected systemically in four animals; four control animals received dextrose 5%. Monkeys were examined by slit-lamp biomicroscopy and underwent color photography and fluorescein angiography. RESULTS: Group 1: All eyes, treated and control, developed intense and persistent rubeosis iridis. Group 2: Two of the four treated eyes in this group developed minimal iris neovascularization; the other two had no iris neovascularization. All four control eyes developed intense, persistent iris neovascularization. Group 3: All eyes developed extensive rubeosis iridis; iris neovascularization regressed in all four treated eyes after squalamine injections. Two of four treated eyes retained minimal iris neovascularization; two showed complete regression of rubeosis iridis. Rubeosis iridis completely regressed in two of the four control eyes; the remaining two control eyes had intense, persistent iris neovascularization. CONCLUSIONS: Intravitreally injected squalamine did not affect the development of iris neovascularization; however, systemic squalamine injection inhibited the development of iris neovascularization and caused partial regression of new vessels in a primate model.
机译:目的:探讨角鲨胺(一种抗血管生成的氨基固醇)在虹膜新生血管形成实验模型中的作用。方法:通过用氩激光阻塞视网膜静脉并用中央角膜缝合线诱发持续性低渗,在食蟹猴中产生虹膜新血管形成。三组治疗二十四只眼。在第1组中,在静脉阻塞后(第1天)立即向玻璃体内注射3 microg / 0.1 mL角鲨胺和4只眼睛,并用平衡盐溶液(对照组)注射。每3天重复注射3周。在第2组中,对四只动物静脉内输注1 mg / kg角鲨胺,并用5%葡萄糖对其进行静脉输注。四只对照动物仅接受葡萄糖。从第1天开始输注,每3天重复一次,持续3周。在第3组中,在第7天虹膜新生血管形成后,对四只动物全身注射1 mg / kg角鲨胺。四只对照动物接受5%的葡萄糖。通过裂隙灯生物显微镜检查猴子,并进行彩色照相和荧光素血管造影。结果:第1组:所有眼睛,经过治疗和控制,均发展为强烈而持续的虹膜红斑病。第2组:该组四只经治疗的眼睛中有两只出现了最小的虹膜新血管形成。另外两个没有虹膜新生血管。四只对照眼均出现强烈的持续性虹膜新生血管。第三组:所有人的眼睛发展为虹膜广泛性红润。角鲨胺注射后,所有四只经治疗的眼虹膜新生血管均消退。四只经治疗的眼睛中有两只保留了最小的虹膜新生血管。两个显示虹膜红肿完全消退。虹膜红斑病在四只对照眼中的两只完全消失。其余两只对照眼有强烈的持续性虹膜新生血管。结论:玻璃体内注射角鲨胺不影响虹膜新生血管的形成。然而,在灵长类动物模型中,全身性角鲨胺注射抑制了虹膜新生血管的形成,并导致了新血管的部分消退。

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