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Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs

PURPOSE: In guinea pigs, choroidal thickness (ChT) and choroidal blood perfusion (ChBP) simultaneously decrease in experimental myopia, and both increase during recovery. However, the causal relationship between ChBP and myopia requires further investigation. In this study, we examined the changes o...

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Autores principales: Zhou, Xuan, Zhang, Sen, Zhang, Guoyun, Chen, Yizhong, Lei, Yi, Xiang, Jing, Xu, Renchang, Qu, Jia, Zhou, Xiangtian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Association for Research in Vision and Ophthalmology 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7683853/
https://www.ncbi.nlm.nih.gov/pubmed/33211066
http://dx.doi.org/10.1167/iovs.61.13.25
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author Zhou, Xuan
Zhang, Sen
Zhang, Guoyun
Chen, Yizhong
Lei, Yi
Xiang, Jing
Xu, Renchang
Qu, Jia
Zhou, Xiangtian
author_facet Zhou, Xuan
Zhang, Sen
Zhang, Guoyun
Chen, Yizhong
Lei, Yi
Xiang, Jing
Xu, Renchang
Qu, Jia
Zhou, Xiangtian
author_sort Zhou, Xuan
collection PubMed
description PURPOSE: In guinea pigs, choroidal thickness (ChT) and choroidal blood perfusion (ChBP) simultaneously decrease in experimental myopia, and both increase during recovery. However, the causal relationship between ChBP and myopia requires further investigation. In this study, we examined the changes of ChBP with three different antimyopia treatments. We also actively increased ChBP to examine the direct effect on myopia development in guinea pigs. METHODS: Experiment 1: Guinea pigs wore occluders on the right eye for two weeks to induce form-deprivation myopia (FDM). Simultaneously they received daily antimyopia treatments: peribulbar injections of atropine or apomorphine or exposure to intense light. Experiment 2: The vasodilator prazosin was injected daily into the form-deprivation eyes to increase ChBP during the two-week induction of FDM. Other FDM animals received appropriate control treatments. Changes in refraction, axial length, ChBP, ChT, and hypoxia-labeled pimonidazole adducts in the sclera were measured. RESULTS: The antimyopia treatments atropine, apomorphine, and intense light all significantly inhibited myopia development and the decrease in ChBP. The treatments also reduced scleral hypoxia, as indicated by the decrease in hypoxic signals. Furthermore, actively increasing ChBP with prazosin inhibited the progression of myopia, as well as the increase in axial length and scleral hypoxia. CONCLUSIONS: Our data strongly indicate that increased ChBP attenuates scleral hypoxia, and thereby inhibits the development of myopia. Thus ChBP may be a promising target for myopia retardation. As such, it can serve as an immediate predictor of myopia development as well as a long-term marker of it.
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spelling pubmed-76838532020-11-25 Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs Zhou, Xuan Zhang, Sen Zhang, Guoyun Chen, Yizhong Lei, Yi Xiang, Jing Xu, Renchang Qu, Jia Zhou, Xiangtian Invest Ophthalmol Vis Sci Physiology and Pharmacology PURPOSE: In guinea pigs, choroidal thickness (ChT) and choroidal blood perfusion (ChBP) simultaneously decrease in experimental myopia, and both increase during recovery. However, the causal relationship between ChBP and myopia requires further investigation. In this study, we examined the changes of ChBP with three different antimyopia treatments. We also actively increased ChBP to examine the direct effect on myopia development in guinea pigs. METHODS: Experiment 1: Guinea pigs wore occluders on the right eye for two weeks to induce form-deprivation myopia (FDM). Simultaneously they received daily antimyopia treatments: peribulbar injections of atropine or apomorphine or exposure to intense light. Experiment 2: The vasodilator prazosin was injected daily into the form-deprivation eyes to increase ChBP during the two-week induction of FDM. Other FDM animals received appropriate control treatments. Changes in refraction, axial length, ChBP, ChT, and hypoxia-labeled pimonidazole adducts in the sclera were measured. RESULTS: The antimyopia treatments atropine, apomorphine, and intense light all significantly inhibited myopia development and the decrease in ChBP. The treatments also reduced scleral hypoxia, as indicated by the decrease in hypoxic signals. Furthermore, actively increasing ChBP with prazosin inhibited the progression of myopia, as well as the increase in axial length and scleral hypoxia. CONCLUSIONS: Our data strongly indicate that increased ChBP attenuates scleral hypoxia, and thereby inhibits the development of myopia. Thus ChBP may be a promising target for myopia retardation. As such, it can serve as an immediate predictor of myopia development as well as a long-term marker of it. The Association for Research in Vision and Ophthalmology 2020-11-19 /pmc/articles/PMC7683853/ /pubmed/33211066 http://dx.doi.org/10.1167/iovs.61.13.25 Text en Copyright 2020 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License.
spellingShingle Physiology and Pharmacology
Zhou, Xuan
Zhang, Sen
Zhang, Guoyun
Chen, Yizhong
Lei, Yi
Xiang, Jing
Xu, Renchang
Qu, Jia
Zhou, Xiangtian
Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title_full Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title_fullStr Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title_full_unstemmed Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title_short Increased Choroidal Blood Perfusion Can Inhibit Form Deprivation Myopia in Guinea Pigs
title_sort increased choroidal blood perfusion can inhibit form deprivation myopia in guinea pigs
topic Physiology and Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7683853/
https://www.ncbi.nlm.nih.gov/pubmed/33211066
http://dx.doi.org/10.1167/iovs.61.13.25
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