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Intravitreally-administered dopamine D2-like (and D4), but not D1-like, receptor agonists reduce form-deprivation myopia in tree shrews

Published online by Cambridge University Press:  16 January 2017

ALEXANDER H. WARD*
Affiliation:
Genetics, Genomics and Bioinformatics Theme, University of Alabama at Birmingham, Birmingham, AL 35294
JOHN T. SIEGWART JR.
Affiliation:
Department of Optometry and Vision Science, University of Alabama at Birmingham, Birmingham, AL 35294
MICHAEL R. FROST
Affiliation:
Department of Optometry and Vision Science, University of Alabama at Birmingham, Birmingham, AL 35294
THOMAS T. NORTON
Affiliation:
Department of Optometry and Vision Science, University of Alabama at Birmingham, Birmingham, AL 35294
*
*Address correspondence to: Alexander H. Ward, 302 Worrell Building, University of Alabama at Birmingham, Birmingham, AL 35294-4390. E-mail: alexward@uab.edu
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Abstract

We examined the effect of intravitreal injections of D1-like and D2-like dopamine receptor agonists and antagonists and D4 receptor drugs on form-deprivation myopia (FDM) in tree shrews, mammals closely related to primates. In eleven groups (n = 7 per group), we measured the amount of FDM produced by monocular form deprivation (FD) over an 11-day treatment period. The untreated fellow eye served as a control. Animals also received daily 5 µL intravitreal injections in the FD eye. The reference group received 0.85% NaCl vehicle. Four groups received a higher, or lower, dose of a D1-like receptor agonist (SKF38393) or antagonist (SCH23390). Four groups received a higher, or lower, dose of a D2-like receptor agonist (quinpirole) or antagonist (spiperone). Two groups received the D4 receptor agonist (PD168077) or antagonist (PD168568). Refractions were measured daily; axial component dimensions were measured on day 1 (before treatment) and day 12. We found that in groups receiving the D1-like receptor agonist or antagonist, the development of FDM and altered ocular component dimensions did not differ from the NaCl group. Groups receiving the D2-like receptor agonist or antagonist at the higher dose developed significantly less FDM and had shorter vitreous chambers than the NaCl group. The D4 receptor agonist, but not the antagonist, was nearly as effective as the D2-like agonist in reducing FDM. Thus, using intravitreally-administered agents, we did not find evidence supporting a role for the D1-like receptor pathway in reducing FDM in tree shrews. The reduction of FDM by the dopamine D2-like agonist supported a role for the D2-like receptor pathway in the control of FDM. The reduction of FDM by the D4 receptor agonist, but not the D4 antagonist, suggests an important role for activation of the dopamine D4 receptor in the control of axial elongation and refractive development.

Information

Type
Research Article
Copyright
Copyright © Cambridge University Press 2017 
Figure 0

Table 1. Dopamine agonists and antagonists.

Figure 1

Fig. 1. Waveform of retina and choroid. Waveform produced by the Lenstar optical biometer in the control eye of a tree shrew. (A) indicates the anterior surface of the retina. (B) indicates the posterior retina/front of the choroid. (C) marks the back of the choroid. In this example, the retinal thickness, from (A to B), was 173 µm. The choroidal thickness (B to C) was 52 µm.

Figure 2

Fig. 2. Development of FDM and day 12 measures in the NaCl and the D1-like receptor agonist and antagonist groups. (A) The refractive difference (treated eye–control eye) throughout the 11-day period of FD and daily administration of the D1-like receptor agonist or antagonist. The first measure (day 1) was made immediately before the first intravitreal injection and the start of FD; the day 12 measures were made 24 h after the last intravitreal injection. (B) Refractive differences on day 12. (C) Elongation of the vitreous chamber on day 12. Error bars indicate standard error of the mean (s.e.m.). The color of each bar in (B) and (C) matches the symbol color in (A). Abbreviations: SKF = SKF38393, SCH = SCH23390, Ag = agonist, An = antagonist, LD = lower dose, HD = higher dose.

Figure 3

Fig. 3. Development of FDM and day 12 measures in the NaCl and the D2-like receptor agonist and antagonist groups. (A) The refractive difference (treated eye–control eye) throughout the 11-day period of FD and daily administration of dopamine D2-like receptor agonists or antagonists. The first measure (day 1) was made immediately before the first intravitreal injection and the start of FD. The final measure (day 12) was made 24 h after the last intravitreal injection. The refractive response to continued FD, without injections, is shown to the right of the vertical line at 35 DVE. N = number of animals in which myopia development was followed post-injection (after the intravitreal injections ceased). (B) Refractive differences on day 12. (C) Elongation of the vitreous chamber on day 12. Error bars indicate standard error of the mean (s.e.m.). The color of each bar in (B) and (C) matches the symbol color in (A). Asterisks (*) in (B) and (C) indicate significant differences between the higher-dose groups and the NaCl group. Crosses (†) in (B) and (C) indicate that the lower-dose groups were significantly different from the higher-dose groups. Abbreviations: Quin = quinpirole, Spip = spiperone, Ag = agonist, An = antagonist, LD = lower dose, HD = higher dose, Post = post-injection.

Figure 4

Fig. 4. Development of FDM and vitreous chamber depth in the NaCl and the D4 receptor agonist and antagonist groups. (A) The refractive difference (treated eye–control eye) throughout the 11-day period of FD and daily administration of dopamine D4 receptor agonist or antagonist. The first measure (day 1), was made immediately before the first intravitreal injection and the start of FD. The final measure (day 12) was made 24 h after the last intravitreal injection. The refractive response to continued FD, without injections, is shown to the right of the orange vertical line. Asterisks (*) indicate days on which the amount of myopia in the D4 agonist (PD168077) group differed significantly from the myopia in the NaCl group. Crosses (†) indicate significant differences between the D4 agonist (PD168077) group and the D4 antagonist (PD168568) group. N = number of animals in which myopia development was followed post-injection (after the intravitreal injections ceased, starting at day 12). (B) Refractive differences on day 12. (C) Elongation of the vitreous chamber on day 12. Error bars indicate standard error of the mean (s.e.m.). The color of each bar in (B) and (C) matches the symbol color in (A). Abbreviations: Ag = agonist, An = antagonist, Post = post-injection.

Figure 5

Fig. 5. Refractive responses of individual animals in the D4 agonist group. (A) Five of the animals. In one animal (circles), FDM was completely blocked. In two animals (squares and diamonds), the D4 agonist produced no reduction of FDM. In two other animals (triangles), FDM was substantially reduced. (B) The remaining two animals in which FDM was also substantially reduced, displayed separately for clarity. In both (A) and (B), the refractive response to continued FD, without injections, is shown to the right of the orange vertical lines.