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Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy

We hypothesize that melanocortin receptors (MC) could activate tissue protective circuit in a model of streptozotocin- (STZ-) induced diabetic retinopathy (DR) in mice. At 12–16 weeks after diabetes induction, fluorescein angiography (FAG) revealed an approximate incidence of 80% microvascular chang...

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Autores principales: Rossi, S., Maisto, R., Gesualdo, C., Trotta, M. C., Ferraraccio, F., Kaneva, M. K., Getting, S. J., Surace, E., Testa, F., Simonelli, F., Grieco, P., Merlino, F., Perretti, M., D'Amico, M., Di Filippo, C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4753692/
https://www.ncbi.nlm.nih.gov/pubmed/26949291
http://dx.doi.org/10.1155/2016/7368389
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author Rossi, S.
Maisto, R.
Gesualdo, C.
Trotta, M. C.
Ferraraccio, F.
Kaneva, M. K.
Getting, S. J.
Surace, E.
Testa, F.
Simonelli, F.
Grieco, P.
Merlino, F.
Perretti, M.
D'Amico, M.
Di Filippo, C.
author_facet Rossi, S.
Maisto, R.
Gesualdo, C.
Trotta, M. C.
Ferraraccio, F.
Kaneva, M. K.
Getting, S. J.
Surace, E.
Testa, F.
Simonelli, F.
Grieco, P.
Merlino, F.
Perretti, M.
D'Amico, M.
Di Filippo, C.
author_sort Rossi, S.
collection PubMed
description We hypothesize that melanocortin receptors (MC) could activate tissue protective circuit in a model of streptozotocin- (STZ-) induced diabetic retinopathy (DR) in mice. At 12–16 weeks after diabetes induction, fluorescein angiography (FAG) revealed an approximate incidence of 80% microvascular changes, typical of DR, in the animals, without signs of vascular leakage. Occludin progressively decreased in the retina of mice developing retinopathy. qPCR of murine retina revealed expression of two MC receptors, Mc1r and Mc5r. The intravitreal injection (5 μL) of the selective MC(1) small molecule agonist BMS-470539 (33 μmol) and the MC(5) peptidomimetic agonist PG-901 (7.32 nM) elicited significant protection with regular course and caliber of retinal vessels, as quantified at weeks 12 and 16 after diabetes induction. Mouse retina homogenate settings indicated an augmented release of IL-1α, IL-1β, IL-6, MIP-1α, MIP-2α, MIP-3α, and VEGF from diabetic compared to nondiabetic mice. Application of PG20N or AGRP and MC(5) and MC(1) antagonist, respectively, augmented the release of cytokines, while the agonists BMS-470539 and PG-901 almost restored normal pattern of these mediators back to nondiabetic values. Similar changes were quantified with respect to Ki-67 staining. Finally, application of MC(3)-MC(4) agonist/antagonists resulted to be inactive with respect to all parameters under assessment.
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spelling pubmed-47536922016-03-06 Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy Rossi, S. Maisto, R. Gesualdo, C. Trotta, M. C. Ferraraccio, F. Kaneva, M. K. Getting, S. J. Surace, E. Testa, F. Simonelli, F. Grieco, P. Merlino, F. Perretti, M. D'Amico, M. Di Filippo, C. Mediators Inflamm Research Article We hypothesize that melanocortin receptors (MC) could activate tissue protective circuit in a model of streptozotocin- (STZ-) induced diabetic retinopathy (DR) in mice. At 12–16 weeks after diabetes induction, fluorescein angiography (FAG) revealed an approximate incidence of 80% microvascular changes, typical of DR, in the animals, without signs of vascular leakage. Occludin progressively decreased in the retina of mice developing retinopathy. qPCR of murine retina revealed expression of two MC receptors, Mc1r and Mc5r. The intravitreal injection (5 μL) of the selective MC(1) small molecule agonist BMS-470539 (33 μmol) and the MC(5) peptidomimetic agonist PG-901 (7.32 nM) elicited significant protection with regular course and caliber of retinal vessels, as quantified at weeks 12 and 16 after diabetes induction. Mouse retina homogenate settings indicated an augmented release of IL-1α, IL-1β, IL-6, MIP-1α, MIP-2α, MIP-3α, and VEGF from diabetic compared to nondiabetic mice. Application of PG20N or AGRP and MC(5) and MC(1) antagonist, respectively, augmented the release of cytokines, while the agonists BMS-470539 and PG-901 almost restored normal pattern of these mediators back to nondiabetic values. Similar changes were quantified with respect to Ki-67 staining. Finally, application of MC(3)-MC(4) agonist/antagonists resulted to be inactive with respect to all parameters under assessment. Hindawi Publishing Corporation 2016 2016-01-12 /pmc/articles/PMC4753692/ /pubmed/26949291 http://dx.doi.org/10.1155/2016/7368389 Text en Copyright © 2016 S. Rossi et al. https://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Rossi, S.
Maisto, R.
Gesualdo, C.
Trotta, M. C.
Ferraraccio, F.
Kaneva, M. K.
Getting, S. J.
Surace, E.
Testa, F.
Simonelli, F.
Grieco, P.
Merlino, F.
Perretti, M.
D'Amico, M.
Di Filippo, C.
Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title_full Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title_fullStr Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title_full_unstemmed Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title_short Activation of Melanocortin Receptors MC(1) and MC(5) Attenuates Retinal Damage in Experimental Diabetic Retinopathy
title_sort activation of melanocortin receptors mc(1) and mc(5) attenuates retinal damage in experimental diabetic retinopathy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4753692/
https://www.ncbi.nlm.nih.gov/pubmed/26949291
http://dx.doi.org/10.1155/2016/7368389
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