Glucagon Receptor Agonists and Antagonists Affect the Growth of the Chick Eye: A Role for Glucagonergic Regulation of Emmetropization?
- 1 November 2005
- journal article
- Published by Association for Research in Vision and Ophthalmology (ARVO) in Investigative Opthalmology & Visual Science
- Vol. 46 (11) , 3922-3931
- https://doi.org/10.1167/iovs.04-1026
Abstract
Purpose. In chicks, plus defocus retards eye growth, thickens the choroid, and activates glucagonergic amacrine cells, probably releasing glucagon. Glucagon receptor antagonists (expected to inhibit compensation to plus defocus) and agonists (expected to block myopia induction by form deprivation) were administered to eyes of chicks, to test the hypothesis that glucagon mediates the induction of changes in eye growth by plus defocus. methods. Seven-day-old (P7) chick eyes were injected intravitreally with peptides at concentrations of ∼10−9 to 10−5 M in 20 μL (injection volume). The glucagon-receptor antagonists [des-His1,des- Phe 6 ,Glu9]-glucagon-NH2 (des- Phe 6 -antagonist) and [des-His1,Glu9]-glucagon-NH2 (Phe 6 -antagonist) were administered daily for 4 to 5 days to plus-defocused eyes. Agonists (porcine glucagon-[1-29] and [Lys17,18,Glu21]-glucagon-NH2) were monocularly administered daily for 5 days to form-deprived eyes. The contralateral eye remained open and received saline. After treatment, eyes were refracted, measured, and examined for histologic changes. results. The Phe 6 -antagonist at 10−5 M (in the syringe) inhibited changes in both refractive error and axial length compensation induced by +7-D lens wear; however, des-Phe 6 -antagonist (10−5 M) had weak, inconsistent effects and did not antagonize the action of exogenous glucagon. Glucagon prevented ocular elongation and myopia and induced choroidal thickening in form-deprived eyes. [Lys17,18,Glu21]-glucagon-NH2 had little effect at 10−7 M, but at 10−6 to 10−5 M altered rod structure and inhibited eye growth. conclusions. Exogenous glucagon inhibited the growth of form-deprived eyes, whereas Phe 6 -antagonist inhibited compensation to plus defocus, as might be expected if glucagon is an endogenous mediator of emmetropization. The reason for the failure of des-Phe 6 -antagonist to counteract the effects of exogenous glucagon requires further investigation.Keywords
This publication has 35 references indexed in Scilit:
- Image Defocus Modulates Activity of Bipolar and Amacrine Cells in Macaque RetinaInvestigative Opthalmology & Visual Science, 2004
- Effects of Positive and Negative Lens Treatment on Retinal and Choroidal Glucagon and Glucagon Receptor mRNA Levels in the ChickenInvestigative Opthalmology & Visual Science, 2004
- Variable effects of previously untested muscarinic receptor antagonists on experimental myopia.Investigative Opthalmology & Visual Science, 2003
- International Union of Pharmacology. XXXV. The Glucagon Receptor FamilyPharmacological Reviews, 2003
- Activation of two signal-transduction systems in hepatocytes by glucagonNature, 1986
- Glucagon-like immunoreactivity in mouse and rat retinaNeuroscience Letters, 1985
- GLUCAGON AND VIP IN THE RETINA1985
- The effects of VIP on cyclic AMP and glycogen levels in vertebrate retinaPeptides, 1984
- Glucagon immunoreactive neurons in the retina of different speciesAlbrecht von Graefes Archiv für Ophthalmologie, 1983
- Retinoscopy and Eye SizeScience, 1970