Author:
FELDKAEMPER MARITA P.,SCHAEFFEL FRANK
Abstract
Eye growth and refraction are regulated by visual processing
in the retina. Until now, the messengers released by the retina
to induce these changes are largely unknown. Previously, it
was found that glucagon amacrine cells respond to defocus in
the retinal image and even to its sign. The expression of the
immediate-early gene product ZENK increased in this cell population
in eyes wearing plus lenses and decreased in minus lens-treated
chicks. Moreover, it was shown that the amount of retinal glucagon
mRNA increased during treatment with positive lenses. Therefore,
it seems likely that these cells contribute to the visual
regulation of ocular growth and that glucagon may act as a stop
signal for eye growth. The purpose of the present study was
to accumulate further evidence for a role of glucagon in the
visual control of eye growth. Chicks were treated with plus
and minus lenses after injection of different amounts of the
glucagon antagonist des-His1-Glu9-glucagon-amide
or the agonist Lys17,18,Glu21-glucagon,
respectively. Refractive development and eye growth were recorded by
automated infrared photorefraction and A-scan ultrasound, respectively.
The glucagon antagonist inhibited hyperopia development, albeit only in
a narrow concentration range, and at most by 50%, but not myopia
development. In contrast, the agonist inhibited myopia development
in a dose-dependent fashion. At high concentrations, it also
prevented hyperopia development.
Publisher
Cambridge University Press (CUP)
Subject
Sensory Systems,Physiology
Cited by
74 articles.
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