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阿扑吗啡通过作用于视网膜或色素上皮的多巴胺D2受体机制来阻止鸡的形觉剥夺性近视。

Apomorphine blocks form-deprivation myopia in chickens by a dopamine D2-receptor mechanism acting in retina or pigmented epithelium.

作者信息

Rohrer B, Spira A W, Stell W K

机构信息

Department of Anatomy, University of Calgary Faculty of Medicine, Alberta, Canada.

出版信息

Vis Neurosci. 1993 May-Jun;10(3):447-53. doi: 10.1017/s0952523800004673.

DOI:10.1017/s0952523800004673
PMID:8494798
Abstract

Studies of form-deprivation myopia (FDM) in animal models have shown that postnatal ocular growth is regulated by the quality of patterned images on the retina. One of the major challenges in myopia research is to identify the biochemical mechanisms which translate retinal visual responses into signals that regulate scleral growth. Dopamine (DA) has been implicated in this process, since retinal DA levels decline in FDM and subconjunctival injections of apomorphine (Apo, a nonspecific DA agonist) prevent FDM in a dose-dependent way (Stone et al., 1989). To gain insight into where and how DA ligands act to regulate ocular elongation, we compared the action and distribution of DA receptor ligands injected intravitreally vs. subconjunctivally in young chicks. Ocular length was measured by A-scan ultrasound. We found that daily intravitreal injections of Apo block FDM at a 50% effective dose (ED50) of 5 pg per day, or a peak concentration in the vitreous humor of 108 pM, compared to an ED50 of 2.5 ng for subconjunctival injections as reported by Stone et al. (1989, 1990). [3H]-spiperone, a D2-receptor antagonist, reached average maximum retinal concentrations of 160 pM and 260 pM, during the first hour after intravitreal and subconjunctival administration, respectively, at the ED50 dose. In contrast, the maximum spiperone concentrations in the retinal pigment epithelium (RPE) were 30 pM and 410 pM, respectively, after intravitreal or subconjunctival ED50 doses. Spiperone concentrations in sclera after ED50 doses to the two sites differed by 4 x 10(4) (0.4 pM vs. 1.7 nM, respectively).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对动物模型中形觉剥夺性近视(FDM)的研究表明,出生后眼的生长受视网膜上有图案图像质量的调节。近视研究中的主要挑战之一是确定将视网膜视觉反应转化为调节巩膜生长信号的生化机制。多巴胺(DA)参与了这一过程,因为在FDM中视网膜DA水平会下降,而结膜下注射阿扑吗啡(Apo,一种非特异性DA激动剂)能以剂量依赖的方式预防FDM(斯通等人,1989年)。为了深入了解DA配体在何处以及如何发挥作用来调节眼轴伸长,我们比较了玻璃体内注射与结膜下注射DA受体配体在幼雏中的作用和分布。通过A超超声测量眼轴长度。我们发现,每天玻璃体内注射Apo以每天5 pg的50%有效剂量(ED50)或玻璃体液中108 pM的峰值浓度可阻断FDM,相比之下,斯通等人(1989年、1990年)报道结膜下注射的ED50为2.5 ng。在ED50剂量下,D2受体拮抗剂[3H] - 螺哌隆在玻璃体内和结膜下给药后的第一小时分别达到视网膜平均最大浓度160 pM和260 pM。相比之下,在玻璃体内或结膜下ED50剂量后,视网膜色素上皮(RPE)中的螺哌隆最大浓度分别为30 pM和410 pM。在ED50剂量下,向两个部位给药后巩膜中的螺哌隆浓度相差4×10⁴(分别为0.4 pM和1.7 nM)。(摘要截取自250字)

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