| Literature DB >> 33318177 |
Jeffrey M Harder1, Chelsea Guymer2, John P M Wood2, Evangelia Daskalaki3, Glyn Chidlow2, Chi Zhang4,5,6, Revathi Balasubramanian4,5,6, Brynn H Cardozo1, Nicole E Foxworth1, Kelly E Deering1, Tionna B Ouellette1, Christa Montgomery4,5,6, Craig E Wheelock3, Robert J Casson2, Pete A Williams7, Simon W M John8,4,5,6.
Abstract
Intraocular pressure-sensitive retinal ganglion cell degeneration is a hallmark of glaucoma, the leading cause of irreversible blindness. Here, we used RNA-sequencing and metabolomics to examine early glaucoma in DBA/2J mice. We demonstrate gene expression changes that significantly impact pathways mediating the metabolism and transport of glucose and pyruvate. Subsequent metabolic studies characterized an intraocular pressure (IOP)-dependent decline in retinal pyruvate levels coupled to dysregulated glucose metabolism prior to detectable optic nerve degeneration. Remarkably, retinal glucose levels were elevated 50-fold, consistent with decreased glycolysis but possibly including glycogen mobilization and other metabolic changes. Oral supplementation of the glycolytic product pyruvate strongly protected from neurodegeneration in both rat and mouse models of glaucoma. Investigating further, we detected mTOR activation at the mechanistic nexus of neurodegeneration and metabolism. Rapamycin-induced inhibition of mTOR robustly prevented glaucomatous neurodegeneration, supporting a damaging role for IOP-induced mTOR activation in perturbing metabolism and promoting glaucoma. Together, these findings support the use of treatments that limit metabolic disturbances and provide bioenergetic support. Such treatments provide a readily translatable strategy that warrants investigation in clinical trials.Entities:
Keywords: glaucoma; neuronal metabolism; neuroprotection; pyruvate; retinal ganglion cell
Year: 2020 PMID: 33318177 DOI: 10.1073/pnas.2014213117
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205