Molecular clustering identifies complement and endothelin induction as early events in a mouse model of glaucoma
Gareth R. Howell, … , Richard T. Libby, Simon W.M. John
Gareth R. Howell, … , Richard T. Libby, Simon W.M. John
Published March 7, 2011
Citation Information: J Clin Invest. 2011;121(4):1429-1444. https://doi.org/10.1172/JCI44646.
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Research Article Ophthalmology

Molecular clustering identifies complement and endothelin induction as early events in a mouse model of glaucoma

Abstract

Glaucoma is one of the most common neurodegenerative diseases. Despite this, the earliest stages of this complex disease are still unclear. This study was specifically designed to identify early stages of glaucoma in DBA/2J mice. To do this, we used genome-wide expression profiling of optic nerve head and retina and a series of computational methods. Eyes with no detectable glaucoma by conventional assays were grouped into molecularly defined stages of disease using unbiased hierarchical clustering. These stages represent a temporally ordered sequence of glaucoma states. We then determined networks and biological processes that were altered at these early stages. Early-stage expression changes included upregulation of both the complement cascade and the endothelin system, and so we tested the therapeutic value of separately inhibiting them. Mice with a mutation in complement component 1a (C1qa) were protected from glaucoma. Similarly, inhibition of the endothelin system with bosentan, an endothelin receptor antagonist, was strongly protective against glaucomatous damage. Since endothelin 2 is potently vasoconstrictive and was produced by microglia/macrophages, our data provide what we believe to be a novel link between these cell types and vascular dysfunction in glaucoma. Targeting early molecular events, such as complement and endothelin induction, may provide effective new treatments for human glaucoma.

Authors

Gareth R. Howell, Danilo G. Macalinao, Gregory L. Sousa, Michael Walden, Ileana Soto, Stephen C. Kneeland, Jessica M. Barbay, Benjamin L. King, Jeffrey K. Marchant, Matthew Hibbs, Beth Stevens, Ben A. Barres, Abbot F. Clark, Richard T. Libby, Simon W.M. John

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Figure 10

Bosentan robustly protects from glaucoma in DBA/2J glaucoma.

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Bosentan robustly protects from glaucoma in DBA/2J glaucoma. (A) Adminis...
(A) Administration of bosentan (an endothelin receptor antagonist) does not alter IOP elevation in DBA/2J mice. Sample size: 39–47 per group. (B) Bosentan administration protects significant numbers of eyes from glaucoma (10.5 months, P = 1 × 10–26; 12 months, P = 0.01; sample sizes: 54 untreated, 54 treated at 10.5 months and 58 untreated, 58 treated at 12 months). (C) Randomly selected mice that were treated with bosentan and had the NOE nerve damage level have an axon number similar to that in no-glaucoma Gpnmb+ controls (11 treated vs. 13 Gpnmb+, P = 0.5) and in DBA/2J mice prior to glaucomatous axon loss. For ease of comparison, axon counts for stages 1–5 are repeated from Figure 1. (D) There is no significant soma loss in bosentan-protected eyes (NOE). Not unexpectedly, Bosentan did not save RGC soma in eyes with severe axon loss (SEV). (E) Representative optic nerve and retinal phenotypes for mice of each treatment group are shown. Optic nerve cross sections were stained with PPD; retinas with cresyl violet. Scale bar: 50 μm.