Profiling IOP-Responsive Genes in the Trabecular Meshwork and Optic Nerve Head in a Rat Model of Controlled Elevation of Intraocular Pressure.
Lozano Diana C, Yang Yong-Feng, Cepurna William O, Smoody Barbara F, Ing Eliesa, Morrison John C, Keller Kate E
AI Summary
This rat study found elevated IOP alters gene expression in the trabecular meshwork (TGFβ pathway downregulated) and optic nerve head (immune/defense pathways upregulated), suggesting distinct tissue responses to pressure that may impact glaucoma.
Abstract
Purpose
The rat controlled elevation of intraocular pressure (CEI) model allows study of in vivo responses to short-term exposure to defined intraocular pressures (IOP). In this study, we used NanoString technology to investigate in vivo IOP-related gene responses in the trabecular meshwork (TM) and optic nerve head (ONH) simultaneously from the same animals.
Methods
Male and female rats (N = 35) were subjected to CEI for 8 hours at pressures simulating mean, daytime normotensive rat IOP (CEI-20), or 2.5× IOP (CEI-50). Naïve animals that received no anesthesia or surgical interventions served as controls. Immediately after CEI, TM and ONH tissues were dissected, RNA was isolated, and samples were analyzed with a NanoString panel containing 770 genes. Postprocessing, raw count data were uploaded to ROSALIND for differential gene expression analyses.
Results
For the TM, 45 IOP-related genes were significant in the CEI-50 versus CEI-20 and CEI-50 versus naïve comparisons, with 15 genes common to both comparisons. Bioinformatics analysis identified Notch and transforming growth factor beta (TGFβ) pathways to be the most up- and downregulated Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways, respectively. For ONH, 22 significantly differentially regulated genes were identified in the CEI-50 versus naïve comparison. Pathway analysis identified defense response and immune response as two significantly upregulated biological process pathways.
Conclusions
This study demonstrated the ability to assay short-term IOP-responsive genes in both TM and ONH tissues simultaneously. In the TM, downregulation of TGFβ pathway genes suggests that TM responses may reduce TGFβ-induced extracellular matrix synthesis. For ONH, the initial response to short-term elevated IOP may be protective.
MeSH Terms
Shields Classification
Key Concepts5
In male and female rats (N = 35) subjected to controlled elevation of intraocular pressure (CEI) for 8 hours at 2.5x IOP (CEI-50) compared to CEI-20 (mean, daytime normotensive rat IOP), 45 IOP-related genes were significant in the trabecular meshwork (TM).
In male and female rats (N = 35) subjected to controlled elevation of intraocular pressure (CEI) for 8 hours at 2.5x IOP (CEI-50) compared to naive animals, 45 IOP-related genes were significant in the trabecular meshwork (TM).
Bioinformatics analysis of gene expression in the trabecular meshwork of male and female rats (N = 35) subjected to controlled elevation of intraocular pressure (CEI-50) identified the Notch pathway as the most upregulated and the transforming growth factor beta (TGFβ) pathway as the most downregulated Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways.
In the optic nerve head (ONH) of male and female rats (N = 35) subjected to controlled elevation of intraocular pressure (CEI) for 8 hours at 2.5x IOP (CEI-50) compared to naive animals, 22 significantly differentially regulated genes were identified.
Pathway analysis of gene expression in the optic nerve head (ONH) of male and female rats (N = 35) subjected to controlled elevation of intraocular pressure (CEI-50) identified defense response and immune response as two significantly upregulated biological process pathways.
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