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多巴胺拮抗剂和短暂视觉刺激可区分晶状体诱导性近视和形觉剥夺性近视。

Dopamine antagonists and brief vision distinguish lens-induced- and form-deprivation-induced myopia.

出版信息

Exp Eye Res. 2011 Nov;93(5):782-5. doi: 10.1016/j.exer.2011.08.001. Epub 2011 Aug 23.

Abstract

In eyes wearing negative lenses, the D2 dopamine antagonist spiperone was only partly effective in preventing the ameliorative effects of brief periods of vision (Nickla et al., 2010), in contrast to reports from studies using form-deprivation. The present study was done to directly compare the effects of spiperone, and the D1 antagonist SCH-23390, on the two different myopiagenic paradigms. 12-day old chickens wore monocular diffusers (form-deprivation) or -10 D lenses attached to the feathers with matching rings of Velcro. Each day for 4 days, 10 μl intravitreal injections of the dopamine D2/D4 antagonist spiperone (5 nmoles) or the D1 antagonist SCH-23390, were given under isoflurane anesthesia, and the diffusers (n = 16; n = 5, respectively) or lenses (n = 20; n = 6) were removed for 2 h immediately after. Saline injections prior to vision were done as controls (form-deprivation: n = 11; lenses: n = 10). Two other saline-injected groups wore the lenses (n = 12) or diffusers (n = 4) continuously. Axial dimensions were measured by high frequency A-scan ultrasonography at the start, and on the last day immediately prior to, and 3 h after the injection. Refractive errors were measured at the end of the experiment using a Hartinger's refractometer. In form-deprived eyes, spiperone, but not SCH-23390, prevented the ocular growth inhibition normally effected by the brief periods of vision (change in vitreous chamber depth, spiperone vs saline: 322 vs 211 μm; p = 0.01). By contrast, neither had any effect on negative lens-wearing eyes given similar unrestricted vision (210 and 234 μm respectively, vs 264 μm). The increased elongation in the spiperone-injected form-deprived eyes did not, however, result in a myopic shift, probably due to the inhibitory effect of the drug on anterior chamber growth (drug vs saline: 96 vs 160 μm; p < 0.01). Finally, spiperone inhibited the vision-induced transient choroidal thickening in form-deprived eyes, while SCH-23390 did not. These results indicate that the dopaminergic mechanisms mediating the protective effects of brief periods of unrestricted vision differ for form-deprivation versus negative lens-wear, which may imply different growth control mechanisms between the two.

摘要

在佩戴负透镜的眼睛中,D2 多巴胺拮抗剂 spiperone 仅部分有效预防短暂视觉时期的改善效果(Nickla 等人,2010 年),这与使用形态剥夺的研究报告相反。本研究旨在直接比较 spiperone 和 D1 拮抗剂 SCH-23390 对两种不同的近视发生范式的影响。12 日龄的鸡佩戴单眼扩散器(形态剥夺)或与 Velcro 匹配的环连接的-10 D 透镜。每天 4 天,在异氟烷麻醉下给予 10 μl 眼内注射多巴胺 D2/D4 拮抗剂 spiperone(5nmoles)或 D1 拮抗剂 SCH-23390,并在立即去除扩散器(n = 16;n = 5,分别)或透镜(n = 20;n = 6)2 小时后。在进行视觉之前进行盐水注射作为对照(形态剥夺:n = 11;镜片:n = 10)。另外两个连续接受盐水注射的组佩戴镜片(n = 12)或扩散器(n = 4)。在开始时、注射前最后一天以及注射后 3 小时,通过高频 A 扫描超声测量眼轴尺寸。在实验结束时,使用 Hartinger 折射计测量屈光不正。在形态剥夺的眼睛中,spiperone 但不是 SCH-23390 阻止了短暂视觉通常产生的眼球生长抑制(玻璃体腔深度变化,spiperone 与盐水:322 与 211 μm;p = 0.01)。相比之下,在给予类似不受限制的视觉的佩戴负透镜的眼睛中,它们均无任何影响(分别为 210 和 234 μm,而 264 μm)。然而,在注射 spiperone 的形态剥夺眼睛中,增加的伸长并没有导致近视转移,这可能是由于药物对前房生长的抑制作用(药物与盐水:96 与 160 μm;p < 0.01)。最后,spiperone 抑制了形态剥夺引起的短暂脉络膜增厚,而 SCH-23390 则没有。这些结果表明,短暂无限制视觉的保护作用所介导的多巴胺能机制在形态剥夺与负透镜佩戴之间存在差异,这可能意味着两种机制之间存在不同的生长控制机制。

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