Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity

Increased exposure to blue or visible light, fluctuations in oxygen tension, and the excessive accumulation of toxic retinoid byproducts places a tremendous amount of stress on the retina. Reduction of visual chromophore biosynthesis may be an effective method to reduce the impact of these stressors...

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Autores principales: Bavik, Claes, Henry, Susan Hayes, Zhang, Yan, Mitts, Kyoko, McGinn, Tim, Budzynski, Ewa, Pashko, Andriy, Lieu, Kuo Lee, Zhong, Sheng, Blumberg, Bruce, Kuksa, Vladimir, Orme, Mark, Scott, Ian, Fawzi, Ahmad, Kubota, Ryo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4430241/
https://www.ncbi.nlm.nih.gov/pubmed/25970164
http://dx.doi.org/10.1371/journal.pone.0124940
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author Bavik, Claes
Henry, Susan Hayes
Zhang, Yan
Mitts, Kyoko
McGinn, Tim
Budzynski, Ewa
Pashko, Andriy
Lieu, Kuo Lee
Zhong, Sheng
Blumberg, Bruce
Kuksa, Vladimir
Orme, Mark
Scott, Ian
Fawzi, Ahmad
Kubota, Ryo
author_facet Bavik, Claes
Henry, Susan Hayes
Zhang, Yan
Mitts, Kyoko
McGinn, Tim
Budzynski, Ewa
Pashko, Andriy
Lieu, Kuo Lee
Zhong, Sheng
Blumberg, Bruce
Kuksa, Vladimir
Orme, Mark
Scott, Ian
Fawzi, Ahmad
Kubota, Ryo
author_sort Bavik, Claes
collection PubMed
description Increased exposure to blue or visible light, fluctuations in oxygen tension, and the excessive accumulation of toxic retinoid byproducts places a tremendous amount of stress on the retina. Reduction of visual chromophore biosynthesis may be an effective method to reduce the impact of these stressors and preserve retinal integrity. A class of non-retinoid, small molecule compounds that target key proteins of the visual cycle have been developed. The first candidate in this class of compounds, referred to as visual cycle modulators, is emixustat hydrochloride (emixustat). Here, we describe the effects of emixustat, an inhibitor of the visual cycle isomerase (RPE65), on visual cycle function and preservation of retinal integrity in animal models. Emixustat potently inhibited isomerase activity in vitro (IC(50) = 4.4 nM) and was found to reduce the production of visual chromophore (11-cis retinal) in wild-type mice following a single oral dose (ED(50) = 0.18 mg/kg). Measure of drug effect on the retina by electroretinography revealed a dose-dependent slowing of rod photoreceptor recovery (ED(50) = 0.21 mg/kg) that was consistent with the pattern of visual chromophore reduction. In albino mice, emixustat was shown to be effective in preventing photoreceptor cell death caused by intense light exposure. Pre-treatment with a single dose of emixustat (0.3 mg/kg) provided a ~50% protective effect against light-induced photoreceptor cell loss, while higher doses (1–3 mg/kg) were nearly 100% effective. In Abca4-/- mice, an animal model of excessive lipofuscin and retinoid toxin (A2E) accumulation, chronic (3 month) emixustat treatment markedly reduced lipofuscin autofluorescence and reduced A2E levels by ~60% (ED(50) = 0.47 mg/kg). Finally, in the retinopathy of prematurity rodent model, treatment with emixustat during the period of ischemia and reperfusion injury produced a ~30% reduction in retinal neovascularization (ED(50) = 0.46mg/kg). These data demonstrate the ability of emixustat to modulate visual cycle activity and reduce pathology associated with various biochemical and environmental stressors in animal models. Other attributes of emixustat, such as oral bioavailability and target specificity make it an attractive candidate for clinical development in the treatment of retinal disease.
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spelling pubmed-44302412015-05-21 Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity Bavik, Claes Henry, Susan Hayes Zhang, Yan Mitts, Kyoko McGinn, Tim Budzynski, Ewa Pashko, Andriy Lieu, Kuo Lee Zhong, Sheng Blumberg, Bruce Kuksa, Vladimir Orme, Mark Scott, Ian Fawzi, Ahmad Kubota, Ryo PLoS One Research Article Increased exposure to blue or visible light, fluctuations in oxygen tension, and the excessive accumulation of toxic retinoid byproducts places a tremendous amount of stress on the retina. Reduction of visual chromophore biosynthesis may be an effective method to reduce the impact of these stressors and preserve retinal integrity. A class of non-retinoid, small molecule compounds that target key proteins of the visual cycle have been developed. The first candidate in this class of compounds, referred to as visual cycle modulators, is emixustat hydrochloride (emixustat). Here, we describe the effects of emixustat, an inhibitor of the visual cycle isomerase (RPE65), on visual cycle function and preservation of retinal integrity in animal models. Emixustat potently inhibited isomerase activity in vitro (IC(50) = 4.4 nM) and was found to reduce the production of visual chromophore (11-cis retinal) in wild-type mice following a single oral dose (ED(50) = 0.18 mg/kg). Measure of drug effect on the retina by electroretinography revealed a dose-dependent slowing of rod photoreceptor recovery (ED(50) = 0.21 mg/kg) that was consistent with the pattern of visual chromophore reduction. In albino mice, emixustat was shown to be effective in preventing photoreceptor cell death caused by intense light exposure. Pre-treatment with a single dose of emixustat (0.3 mg/kg) provided a ~50% protective effect against light-induced photoreceptor cell loss, while higher doses (1–3 mg/kg) were nearly 100% effective. In Abca4-/- mice, an animal model of excessive lipofuscin and retinoid toxin (A2E) accumulation, chronic (3 month) emixustat treatment markedly reduced lipofuscin autofluorescence and reduced A2E levels by ~60% (ED(50) = 0.47 mg/kg). Finally, in the retinopathy of prematurity rodent model, treatment with emixustat during the period of ischemia and reperfusion injury produced a ~30% reduction in retinal neovascularization (ED(50) = 0.46mg/kg). These data demonstrate the ability of emixustat to modulate visual cycle activity and reduce pathology associated with various biochemical and environmental stressors in animal models. Other attributes of emixustat, such as oral bioavailability and target specificity make it an attractive candidate for clinical development in the treatment of retinal disease. Public Library of Science 2015-05-13 /pmc/articles/PMC4430241/ /pubmed/25970164 http://dx.doi.org/10.1371/journal.pone.0124940 Text en © 2015 Bavik et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Bavik, Claes
Henry, Susan Hayes
Zhang, Yan
Mitts, Kyoko
McGinn, Tim
Budzynski, Ewa
Pashko, Andriy
Lieu, Kuo Lee
Zhong, Sheng
Blumberg, Bruce
Kuksa, Vladimir
Orme, Mark
Scott, Ian
Fawzi, Ahmad
Kubota, Ryo
Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title_full Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title_fullStr Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title_full_unstemmed Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title_short Visual Cycle Modulation as an Approach toward Preservation of Retinal Integrity
title_sort visual cycle modulation as an approach toward preservation of retinal integrity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4430241/
https://www.ncbi.nlm.nih.gov/pubmed/25970164
http://dx.doi.org/10.1371/journal.pone.0124940
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