Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity

PURPOSE: Keratoconus (KC) is characterized by progressive vision loss due to corneal thinning and structural abnormalities. It is hypothesized that KC is caused by deregulated collagen levels and collagen fibril-maturating enzyme lysyl oxidase (LOX). Further, it is currently not understood whether t...

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Autores principales: Shetty, Rohit, Sathyanarayanamoorthy, Arunapriya, Ramachandra, Reshma Airody, Arora, Vishal, Ghosh, Anuprita, Srivatsa, Purnima Raman, Pahuja, Natasha, Nuijts, Rudy M. M. A., Sinha-Roy, Abhijit, Mohan, Rajiv R., Ghosh, Arkasubhra
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4301596/
https://www.ncbi.nlm.nih.gov/pubmed/25593510
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author Shetty, Rohit
Sathyanarayanamoorthy, Arunapriya
Ramachandra, Reshma Airody
Arora, Vishal
Ghosh, Anuprita
Srivatsa, Purnima Raman
Pahuja, Natasha
Nuijts, Rudy M. M. A.
Sinha-Roy, Abhijit
Mohan, Rajiv R.
Ghosh, Arkasubhra
author_facet Shetty, Rohit
Sathyanarayanamoorthy, Arunapriya
Ramachandra, Reshma Airody
Arora, Vishal
Ghosh, Anuprita
Srivatsa, Purnima Raman
Pahuja, Natasha
Nuijts, Rudy M. M. A.
Sinha-Roy, Abhijit
Mohan, Rajiv R.
Ghosh, Arkasubhra
author_sort Shetty, Rohit
collection PubMed
description PURPOSE: Keratoconus (KC) is characterized by progressive vision loss due to corneal thinning and structural abnormalities. It is hypothesized that KC is caused by deregulated collagen levels and collagen fibril-maturating enzyme lysyl oxidase (LOX). Further, it is currently not understood whether the gene expression deregulated by the corneal epithelium influences KC pathogenesis. We studied (i) the expressions of the LOX, collagen I (COL IA1), collagen IV (COL IVA1), MMP9, and IL6 genes in KC corneal epithelia, (ii) validated their expression levels in patient tissues, and (iii) correlated expression levels with KC disease severity. The primary goal of this study was to evaluate the importance of these genes in the progression of KC. METHODS: We analyzed the gene expression levels of the key proteins LOX, collagens (COL IA1 and COL IVA1), MMP9, and IL6 in debrided corneal epithelia from a large cohort of KC patients (90 eyes) and compared them to control patients (52 eyes) without KC. We measured the total LOX activity in the tears of KC patients compared to controls. We also correlated the protein expression levels of LOX and collagens by immunohistochemistry (IHC) in primary tissues from KC patients (27 eyes) undergoing keratoplasty compared to healthy donor corneas (15 eyes). RESULTS: We observed a significant reduction in LOX transcript levels in KC corneal epithelia, and LOX activity in KC tears correlated with disease severity. Collagen transcripts were also reduced in KC while MMP9 transcript levels were upregulated and correlated with disease severity. IL6 was moderately increased in KC patients. IHC demonstrated a reduction in the protein expression levels of LOX in the epithelium and collagen IV in the basement membrane of KC patients compared to healthy donor corneas. CONCLUSIONS: The data demonstrates that the structural deformity of the KC cornea may be dependent on reduced expressions of collagens and LOX, as well as on MMP9 elevated by the corneal epithelium.
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spelling pubmed-43015962015-02-12 Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity Shetty, Rohit Sathyanarayanamoorthy, Arunapriya Ramachandra, Reshma Airody Arora, Vishal Ghosh, Anuprita Srivatsa, Purnima Raman Pahuja, Natasha Nuijts, Rudy M. M. A. Sinha-Roy, Abhijit Mohan, Rajiv R. Ghosh, Arkasubhra Mol Vis Research Article PURPOSE: Keratoconus (KC) is characterized by progressive vision loss due to corneal thinning and structural abnormalities. It is hypothesized that KC is caused by deregulated collagen levels and collagen fibril-maturating enzyme lysyl oxidase (LOX). Further, it is currently not understood whether the gene expression deregulated by the corneal epithelium influences KC pathogenesis. We studied (i) the expressions of the LOX, collagen I (COL IA1), collagen IV (COL IVA1), MMP9, and IL6 genes in KC corneal epithelia, (ii) validated their expression levels in patient tissues, and (iii) correlated expression levels with KC disease severity. The primary goal of this study was to evaluate the importance of these genes in the progression of KC. METHODS: We analyzed the gene expression levels of the key proteins LOX, collagens (COL IA1 and COL IVA1), MMP9, and IL6 in debrided corneal epithelia from a large cohort of KC patients (90 eyes) and compared them to control patients (52 eyes) without KC. We measured the total LOX activity in the tears of KC patients compared to controls. We also correlated the protein expression levels of LOX and collagens by immunohistochemistry (IHC) in primary tissues from KC patients (27 eyes) undergoing keratoplasty compared to healthy donor corneas (15 eyes). RESULTS: We observed a significant reduction in LOX transcript levels in KC corneal epithelia, and LOX activity in KC tears correlated with disease severity. Collagen transcripts were also reduced in KC while MMP9 transcript levels were upregulated and correlated with disease severity. IL6 was moderately increased in KC patients. IHC demonstrated a reduction in the protein expression levels of LOX in the epithelium and collagen IV in the basement membrane of KC patients compared to healthy donor corneas. CONCLUSIONS: The data demonstrates that the structural deformity of the KC cornea may be dependent on reduced expressions of collagens and LOX, as well as on MMP9 elevated by the corneal epithelium. Molecular Vision 2015-01-12 /pmc/articles/PMC4301596/ /pubmed/25593510 Text en Copyright © 2015 Molecular Vision. http://creativecommons.org/licenses/by-nc-nd/3.0/ 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 work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Shetty, Rohit
Sathyanarayanamoorthy, Arunapriya
Ramachandra, Reshma Airody
Arora, Vishal
Ghosh, Anuprita
Srivatsa, Purnima Raman
Pahuja, Natasha
Nuijts, Rudy M. M. A.
Sinha-Roy, Abhijit
Mohan, Rajiv R.
Ghosh, Arkasubhra
Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title_full Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title_fullStr Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title_full_unstemmed Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title_short Attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
title_sort attenuation of lysyl oxidase and collagen gene expression in keratoconus patient corneal epithelium corresponds to disease severity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4301596/
https://www.ncbi.nlm.nih.gov/pubmed/25593510
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