Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency

Detalhes bibliográficos
Autor(a) principal: Kobashigawa,Karina Kamachi
Data de Publicação: 2018
Outros Autores: Aldrovani,Marcela, Barros Sobrinho,Alexandre A. F., Silva,Paloma do Espírito Santo, Marcusso,Paulo F., Marinho-Neto,Fausto A., Padua,Ivan R. Martines, Laus,José Luiz
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Arquivos brasileiros de oftalmologia (Online)
Texto Completo: http://old.scielo.br/scielo.php?script=sci_arttext&pid=S0004-27492018000500384
Resumo: ABSTRACT Purposes: To investigate the intra-laboratory reproducibility of clinical features and to evaluate corneal optical anisotropies in a rabbit model of limbal stem cell deficiency. Methods: Limbal injury was induced in the right eye of 23 adult New Zealand White rabbits using a highly aggressive protocol that combined 360 degrees limbal peritomy, keratolimbectomy, alkaline chemical burn, and mechanical removal of the epithelium. Clinical evaluation of the injured eyes was performed for 28 days and included corneal impression cytology. Corneas with a severe clinical outcome set typical of limbal stem cell deficiency were then collected, subjected to a histopathological examination, and examined for optical anisotropies. Corneas from healthy rabbit eyes were used as controls. Differences in optical path due to stromal collagen birefringence, as well as linear dichroism related to the expression and spatial orientation of glycosaminoglycan chains from proteoglycans, were measured from cross-sections under a quantitative polarized light microscope. Results: One eye showed signs of hypopyon and was excluded. Signs of ocular inflammation were observed in all eyes studied (n=22). Corneal impression cytology did not detect goblet cells. Twelve of the 22 corneas presented a clinical outcome set typical of limbal stem cell deficiency, which is characterized by the presence of epithelial defects, inflammatory cells, moderate-to-severe opacity, and neovascularization. Microscopic studies under polarized light revealed that relative to controls, limbal stem cell deficiency caused a 24.4% increase in corneal optical path differences. Further, corneas with limbal stem cell deficiency were less dichroic than controls. Conclusions: These results suggest that rabbit models of limbal stem cell deficiency must be rigorously screened for use in preclinical studies to ensure experimental homogeneity because protocols used to create limbal stem cell deficiency could be not associated with good intra-laboratory reproducibility of clinical features. Limbal stem cell deficiency, as induced herein, altered the optical anisotropic properties of the corneal stroma. Such alterations are indicative of changes in collagen packing and the spatial orientation of glycosaminoglycan chains from proteoglycans. Knowledge of these changes is important to potentiate strategies aimed at restoring the morphofunctional integrity of the corneal stroma affected by limbal stem cell deficiency.
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spelling Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiencyBirefringenceCorneal stromaAnisotropyStem cellsLimbus corneaeGlycosaminoglycansABSTRACT Purposes: To investigate the intra-laboratory reproducibility of clinical features and to evaluate corneal optical anisotropies in a rabbit model of limbal stem cell deficiency. Methods: Limbal injury was induced in the right eye of 23 adult New Zealand White rabbits using a highly aggressive protocol that combined 360 degrees limbal peritomy, keratolimbectomy, alkaline chemical burn, and mechanical removal of the epithelium. Clinical evaluation of the injured eyes was performed for 28 days and included corneal impression cytology. Corneas with a severe clinical outcome set typical of limbal stem cell deficiency were then collected, subjected to a histopathological examination, and examined for optical anisotropies. Corneas from healthy rabbit eyes were used as controls. Differences in optical path due to stromal collagen birefringence, as well as linear dichroism related to the expression and spatial orientation of glycosaminoglycan chains from proteoglycans, were measured from cross-sections under a quantitative polarized light microscope. Results: One eye showed signs of hypopyon and was excluded. Signs of ocular inflammation were observed in all eyes studied (n=22). Corneal impression cytology did not detect goblet cells. Twelve of the 22 corneas presented a clinical outcome set typical of limbal stem cell deficiency, which is characterized by the presence of epithelial defects, inflammatory cells, moderate-to-severe opacity, and neovascularization. Microscopic studies under polarized light revealed that relative to controls, limbal stem cell deficiency caused a 24.4% increase in corneal optical path differences. Further, corneas with limbal stem cell deficiency were less dichroic than controls. Conclusions: These results suggest that rabbit models of limbal stem cell deficiency must be rigorously screened for use in preclinical studies to ensure experimental homogeneity because protocols used to create limbal stem cell deficiency could be not associated with good intra-laboratory reproducibility of clinical features. Limbal stem cell deficiency, as induced herein, altered the optical anisotropic properties of the corneal stroma. Such alterations are indicative of changes in collagen packing and the spatial orientation of glycosaminoglycan chains from proteoglycans. Knowledge of these changes is important to potentiate strategies aimed at restoring the morphofunctional integrity of the corneal stroma affected by limbal stem cell deficiency.Conselho Brasileiro de Oftalmologia2018-10-01info:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersiontext/htmlhttp://old.scielo.br/scielo.php?script=sci_arttext&pid=S0004-27492018000500384Arquivos Brasileiros de Oftalmologia v.81 n.5 2018reponame:Arquivos brasileiros de oftalmologia (Online)instname:Conselho Brasileiro de Oftalmologia (CBO)instacron:CBO10.5935/0004-2749.20180076info:eu-repo/semantics/openAccessKobashigawa,Karina KamachiAldrovani,MarcelaBarros Sobrinho,Alexandre A. F.Silva,Paloma do Espírito SantoMarcusso,Paulo F.Marinho-Neto,Fausto A.Padua,Ivan R. MartinesLaus,José Luizeng2018-08-31T00:00:00Zoai:scielo:S0004-27492018000500384Revistahttp://aboonline.org.br/https://old.scielo.br/oai/scielo-oai.phpaboonline@cbo.com.br||abo@cbo.com.br1678-29250004-2749opendoar:2018-08-31T00:00Arquivos brasileiros de oftalmologia (Online) - Conselho Brasileiro de Oftalmologia (CBO)false
dc.title.none.fl_str_mv Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
title Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
spellingShingle Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
Kobashigawa,Karina Kamachi
Birefringence
Corneal stroma
Anisotropy
Stem cells
Limbus corneae
Glycosaminoglycans
title_short Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
title_full Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
title_fullStr Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
title_full_unstemmed Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
title_sort Clinical features and corneal optical anisotropies in a rabbit model of limbal stem cell deficiency
author Kobashigawa,Karina Kamachi
author_facet Kobashigawa,Karina Kamachi
Aldrovani,Marcela
Barros Sobrinho,Alexandre A. F.
Silva,Paloma do Espírito Santo
Marcusso,Paulo F.
Marinho-Neto,Fausto A.
Padua,Ivan R. Martines
Laus,José Luiz
author_role author
author2 Aldrovani,Marcela
Barros Sobrinho,Alexandre A. F.
Silva,Paloma do Espírito Santo
Marcusso,Paulo F.
Marinho-Neto,Fausto A.
Padua,Ivan R. Martines
Laus,José Luiz
author2_role author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Kobashigawa,Karina Kamachi
Aldrovani,Marcela
Barros Sobrinho,Alexandre A. F.
Silva,Paloma do Espírito Santo
Marcusso,Paulo F.
Marinho-Neto,Fausto A.
Padua,Ivan R. Martines
Laus,José Luiz
dc.subject.por.fl_str_mv Birefringence
Corneal stroma
Anisotropy
Stem cells
Limbus corneae
Glycosaminoglycans
topic Birefringence
Corneal stroma
Anisotropy
Stem cells
Limbus corneae
Glycosaminoglycans
description ABSTRACT Purposes: To investigate the intra-laboratory reproducibility of clinical features and to evaluate corneal optical anisotropies in a rabbit model of limbal stem cell deficiency. Methods: Limbal injury was induced in the right eye of 23 adult New Zealand White rabbits using a highly aggressive protocol that combined 360 degrees limbal peritomy, keratolimbectomy, alkaline chemical burn, and mechanical removal of the epithelium. Clinical evaluation of the injured eyes was performed for 28 days and included corneal impression cytology. Corneas with a severe clinical outcome set typical of limbal stem cell deficiency were then collected, subjected to a histopathological examination, and examined for optical anisotropies. Corneas from healthy rabbit eyes were used as controls. Differences in optical path due to stromal collagen birefringence, as well as linear dichroism related to the expression and spatial orientation of glycosaminoglycan chains from proteoglycans, were measured from cross-sections under a quantitative polarized light microscope. Results: One eye showed signs of hypopyon and was excluded. Signs of ocular inflammation were observed in all eyes studied (n=22). Corneal impression cytology did not detect goblet cells. Twelve of the 22 corneas presented a clinical outcome set typical of limbal stem cell deficiency, which is characterized by the presence of epithelial defects, inflammatory cells, moderate-to-severe opacity, and neovascularization. Microscopic studies under polarized light revealed that relative to controls, limbal stem cell deficiency caused a 24.4% increase in corneal optical path differences. Further, corneas with limbal stem cell deficiency were less dichroic than controls. Conclusions: These results suggest that rabbit models of limbal stem cell deficiency must be rigorously screened for use in preclinical studies to ensure experimental homogeneity because protocols used to create limbal stem cell deficiency could be not associated with good intra-laboratory reproducibility of clinical features. Limbal stem cell deficiency, as induced herein, altered the optical anisotropic properties of the corneal stroma. Such alterations are indicative of changes in collagen packing and the spatial orientation of glycosaminoglycan chains from proteoglycans. Knowledge of these changes is important to potentiate strategies aimed at restoring the morphofunctional integrity of the corneal stroma affected by limbal stem cell deficiency.
publishDate 2018
dc.date.none.fl_str_mv 2018-10-01
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
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dc.identifier.uri.fl_str_mv http://old.scielo.br/scielo.php?script=sci_arttext&pid=S0004-27492018000500384
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dc.language.iso.fl_str_mv eng
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dc.relation.none.fl_str_mv 10.5935/0004-2749.20180076
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dc.publisher.none.fl_str_mv Conselho Brasileiro de Oftalmologia
publisher.none.fl_str_mv Conselho Brasileiro de Oftalmologia
dc.source.none.fl_str_mv Arquivos Brasileiros de Oftalmologia v.81 n.5 2018
reponame:Arquivos brasileiros de oftalmologia (Online)
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reponame_str Arquivos brasileiros de oftalmologia (Online)
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repository.name.fl_str_mv Arquivos brasileiros de oftalmologia (Online) - Conselho Brasileiro de Oftalmologia (CBO)
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