Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush

PURPOSE: A time-course analysis of gene regulation in the adult rat retina after intraorbital nerve crush (IONC) and intraorbital nerve transection (IONT). METHODS: RNA was extracted from adult rat retinas undergoing either IONT or IONC at increasing times post-lesion. Affymetrix RAE230.2 arrays wer...

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Autores principales: Agudo, Marta, Pérez-Marín, Maria Cruz, Lönngren, Ulrika, Sobrado, Paloma, Conesa, Ana, Cánovas, Isabel, Salinas-Navarro, Manuel, Miralles-Imperial, Jaime, Hallböök, Finn, Vidal-Sanz, Manuel
Formato: Texto
Lenguaje:English
Publicado: Molecular Vision 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2426719/
https://www.ncbi.nlm.nih.gov/pubmed/18552980
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author Agudo, Marta
Pérez-Marín, Maria Cruz
Lönngren, Ulrika
Sobrado, Paloma
Conesa, Ana
Cánovas, Isabel
Salinas-Navarro, Manuel
Miralles-Imperial, Jaime
Hallböök, Finn
Vidal-Sanz, Manuel
author_facet Agudo, Marta
Pérez-Marín, Maria Cruz
Lönngren, Ulrika
Sobrado, Paloma
Conesa, Ana
Cánovas, Isabel
Salinas-Navarro, Manuel
Miralles-Imperial, Jaime
Hallböök, Finn
Vidal-Sanz, Manuel
author_sort Agudo, Marta
collection PubMed
description PURPOSE: A time-course analysis of gene regulation in the adult rat retina after intraorbital nerve crush (IONC) and intraorbital nerve transection (IONT). METHODS: RNA was extracted from adult rat retinas undergoing either IONT or IONC at increasing times post-lesion. Affymetrix RAE230.2 arrays were hybridized and analyzed. Statistically regulated genes were annotated and functionally clustered. Arrays were validated by means of quantative reverse transcription polymerase chain reaction (qRT–PCR) on ten regulated genes at two times post-lesion. Western blotting and immunohistofluorescence for four pro-apoptotic proteins were performed on naïve and injured retinas. Finally, custom signaling maps for IONT- and IONC-induced death response were generated (MetaCore, Genego Inc.). RESULTS: Here we show that over time, 3,219 sequences were regulated after IONT and 1,996 after IONC. Out of the total of regulated sequences, 1,078 were commonly regulated by both injuries. Interestingly, while IONT mainly triggers a gene upregulation-sustained over time, IONC causes a transitory downregulation. Functional clustering identified the regulation of high interest biologic processes, most importantly cell death wherein apoptosis was the most significant cluster. Ten death-related genes upregulated by both injuries were used for array validation by means of qRT–PCR. In addition, western blotting and immunohistofluorescence of total and active Caspase 3 (Casp3), tumor necrosis factor receptor type 1 associated death domain (TRADD), tumor necrosis factor receptor superfamily member 1a (TNFR1a), and c-fos were performed to confirm their protein regulation and expression pattern in naïve and injured retinas. These analyses demonstrated that for these genes, protein regulation followed transcriptional regulation and that these pro-apoptotic proteins were expressed by retinal ganglion cells (RGCs). MetaCore-based death-signaling maps show that several apoptotic cascades were regulated in the retina following optic nerve injury and highlight the similarities and differences between IONT and IONC in cell death profiling. CONCLUSIONS: This comprehensive time course retinal transcriptome study comparing IONT and IONC lesions provides a unique valuable tool to understand the molecular mechanisms underlying optic nerve injury and to design neuroprotective protocols.
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spelling pubmed-24267192008-06-13 Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush Agudo, Marta Pérez-Marín, Maria Cruz Lönngren, Ulrika Sobrado, Paloma Conesa, Ana Cánovas, Isabel Salinas-Navarro, Manuel Miralles-Imperial, Jaime Hallböök, Finn Vidal-Sanz, Manuel Mol Vis Research Article PURPOSE: A time-course analysis of gene regulation in the adult rat retina after intraorbital nerve crush (IONC) and intraorbital nerve transection (IONT). METHODS: RNA was extracted from adult rat retinas undergoing either IONT or IONC at increasing times post-lesion. Affymetrix RAE230.2 arrays were hybridized and analyzed. Statistically regulated genes were annotated and functionally clustered. Arrays were validated by means of quantative reverse transcription polymerase chain reaction (qRT–PCR) on ten regulated genes at two times post-lesion. Western blotting and immunohistofluorescence for four pro-apoptotic proteins were performed on naïve and injured retinas. Finally, custom signaling maps for IONT- and IONC-induced death response were generated (MetaCore, Genego Inc.). RESULTS: Here we show that over time, 3,219 sequences were regulated after IONT and 1,996 after IONC. Out of the total of regulated sequences, 1,078 were commonly regulated by both injuries. Interestingly, while IONT mainly triggers a gene upregulation-sustained over time, IONC causes a transitory downregulation. Functional clustering identified the regulation of high interest biologic processes, most importantly cell death wherein apoptosis was the most significant cluster. Ten death-related genes upregulated by both injuries were used for array validation by means of qRT–PCR. In addition, western blotting and immunohistofluorescence of total and active Caspase 3 (Casp3), tumor necrosis factor receptor type 1 associated death domain (TRADD), tumor necrosis factor receptor superfamily member 1a (TNFR1a), and c-fos were performed to confirm their protein regulation and expression pattern in naïve and injured retinas. These analyses demonstrated that for these genes, protein regulation followed transcriptional regulation and that these pro-apoptotic proteins were expressed by retinal ganglion cells (RGCs). MetaCore-based death-signaling maps show that several apoptotic cascades were regulated in the retina following optic nerve injury and highlight the similarities and differences between IONT and IONC in cell death profiling. CONCLUSIONS: This comprehensive time course retinal transcriptome study comparing IONT and IONC lesions provides a unique valuable tool to understand the molecular mechanisms underlying optic nerve injury and to design neuroprotective protocols. Molecular Vision 2008-06-03 /pmc/articles/PMC2426719/ /pubmed/18552980 Text en http://creativecommons.org/licenses/by/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.
spellingShingle Research Article
Agudo, Marta
Pérez-Marín, Maria Cruz
Lönngren, Ulrika
Sobrado, Paloma
Conesa, Ana
Cánovas, Isabel
Salinas-Navarro, Manuel
Miralles-Imperial, Jaime
Hallböök, Finn
Vidal-Sanz, Manuel
Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title_full Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title_fullStr Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title_full_unstemmed Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title_short Time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
title_sort time course profiling of the retinal transcriptome after optic nerve transection and optic nerve crush
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2426719/
https://www.ncbi.nlm.nih.gov/pubmed/18552980
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