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Cellular retinoic acid binding protein-II expression and its potential role in skin aging

Skin aging is an intricate biological process consisting of intrinsic and extrinsic alterations of epidermal and dermal structures. Retinoids play an important role in epidermal cell growth and differentiation and are beneficial to counteract skin aging. Cellular retinoic acid binding protein-II (CR...

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Autores principales: Bielli, Alessandra, Scioli, Maria Giovanna, D’Amico, Federico, Tarquini, Chiara, Agostinelli, Sara, Costanza, Gaetana, Doldo, Elena, Campione, Elena, Passeri, Daniela, Coniglione, Filadelfo, Orlandi, Augusto
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6461173/
https://www.ncbi.nlm.nih.gov/pubmed/30888968
http://dx.doi.org/10.18632/aging.101813
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author Bielli, Alessandra
Scioli, Maria Giovanna
D’Amico, Federico
Tarquini, Chiara
Agostinelli, Sara
Costanza, Gaetana
Doldo, Elena
Campione, Elena
Passeri, Daniela
Coniglione, Filadelfo
Orlandi, Augusto
author_facet Bielli, Alessandra
Scioli, Maria Giovanna
D’Amico, Federico
Tarquini, Chiara
Agostinelli, Sara
Costanza, Gaetana
Doldo, Elena
Campione, Elena
Passeri, Daniela
Coniglione, Filadelfo
Orlandi, Augusto
author_sort Bielli, Alessandra
collection PubMed
description Skin aging is an intricate biological process consisting of intrinsic and extrinsic alterations of epidermal and dermal structures. Retinoids play an important role in epidermal cell growth and differentiation and are beneficial to counteract skin aging. Cellular retinoic acid binding protein-II (CRABP-II) selectively binds all trans-retinoic acid, the most active retinoid metabolite, contributing to regulate intracytoplasmic retinoid trafficking and keratinocyte differentiation. Immunohistochemistry revealed a reduced epidermal and dermal CRABP-II expression in aged human and mouse skin. To better clarify the role of CRABP-II, we investigated age-related skin changes in CRABP-II knock-out mice. We documented an early reduction of keratinocyte layers, proliferation and differentiation rate, dermal and hypodermal thickness, pilosebaceous units and dermal vascularity in CRABP-II knock-out compared with wild-type mice. Ultrastructural investigation documented reduced number and secretion of epidermal lamellar bodies in CRABP-II knock-out compared with wild-type mice. Cultured CRABP-II knock-out-derived dermal fibroblasts proliferated less and showed reduced levels of TGF-β signal-related genes, Col1A1, Col1A2, and increased MMP2 transcripts compared with those from wild-type. Our data strongly support the hypothesis that a reduction of CRABP-II expression accelerates and promotes skin aging, and suggest CRABP-II as a novel target to improve the efficacy of retinoid-mediated anti-aging therapies.
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spelling pubmed-64611732019-04-19 Cellular retinoic acid binding protein-II expression and its potential role in skin aging Bielli, Alessandra Scioli, Maria Giovanna D’Amico, Federico Tarquini, Chiara Agostinelli, Sara Costanza, Gaetana Doldo, Elena Campione, Elena Passeri, Daniela Coniglione, Filadelfo Orlandi, Augusto Aging (Albany NY) Research Paper Skin aging is an intricate biological process consisting of intrinsic and extrinsic alterations of epidermal and dermal structures. Retinoids play an important role in epidermal cell growth and differentiation and are beneficial to counteract skin aging. Cellular retinoic acid binding protein-II (CRABP-II) selectively binds all trans-retinoic acid, the most active retinoid metabolite, contributing to regulate intracytoplasmic retinoid trafficking and keratinocyte differentiation. Immunohistochemistry revealed a reduced epidermal and dermal CRABP-II expression in aged human and mouse skin. To better clarify the role of CRABP-II, we investigated age-related skin changes in CRABP-II knock-out mice. We documented an early reduction of keratinocyte layers, proliferation and differentiation rate, dermal and hypodermal thickness, pilosebaceous units and dermal vascularity in CRABP-II knock-out compared with wild-type mice. Ultrastructural investigation documented reduced number and secretion of epidermal lamellar bodies in CRABP-II knock-out compared with wild-type mice. Cultured CRABP-II knock-out-derived dermal fibroblasts proliferated less and showed reduced levels of TGF-β signal-related genes, Col1A1, Col1A2, and increased MMP2 transcripts compared with those from wild-type. Our data strongly support the hypothesis that a reduction of CRABP-II expression accelerates and promotes skin aging, and suggest CRABP-II as a novel target to improve the efficacy of retinoid-mediated anti-aging therapies. Impact Journals 2019-03-18 /pmc/articles/PMC6461173/ /pubmed/30888968 http://dx.doi.org/10.18632/aging.101813 Text en Copyright © 2019 Bielli et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution (CC BY) 3.0 License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Paper
Bielli, Alessandra
Scioli, Maria Giovanna
D’Amico, Federico
Tarquini, Chiara
Agostinelli, Sara
Costanza, Gaetana
Doldo, Elena
Campione, Elena
Passeri, Daniela
Coniglione, Filadelfo
Orlandi, Augusto
Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title_full Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title_fullStr Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title_full_unstemmed Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title_short Cellular retinoic acid binding protein-II expression and its potential role in skin aging
title_sort cellular retinoic acid binding protein-ii expression and its potential role in skin aging
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6461173/
https://www.ncbi.nlm.nih.gov/pubmed/30888968
http://dx.doi.org/10.18632/aging.101813
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