Abstract

Iron is an essential biometal in the aqueous humor, the principal source of nutrients for the avascular cornea and the lens. Here, we explored whether the ciliary body (CB), the source of aqueous humor, transports iron, and if the prion protein (PrPC) facilitates this process as in the outer retina. Using a combination of human, bovine, and mouse eyes as models, we report the expression of iron export proteins ferroportin and ceruloplasmin, and major iron uptake and storage proteins transferrin, transferrin receptor, and ferritin in the ciliary epithelium, indicating active exchange of iron at this site. Ferroportin and transferrin receptor are also expressed in the corneal endothelium. However, the relative expression of iron export and uptake proteins suggests export from the ciliary epithelium and import by corneal endothelium. In addition, abundant expression of PrPC, a ferrireductase that facilitates iron transport, is noted in pigmented and non-pigmented epithelium of the CB, posterior pigmented epithelium of the iris, corneal endothelium and epithelium, and lens epithelium. Notably, majority of PrPC in the ciliary epithelium is cleaved at the β-site as in retinal pigment epithelial cells, suggesting a role in iron transport. Most of the PrPC in the cornea, however, is full-length, and susceptible to aggregation by intracerebrally inoculated PrP-scrapie, an infectious conformation of PrPC responsible for human and animal prion disorders. Soluble PrPC is present in the aqueous and vitreous humor, a provocative observation with significant implications. Together, these observations suggest independent cycling of iron in the anterior segment, and a prominent role of PrPC in this process. Aggregation of PrPC in the cornea of PrP-scrapie-infected animals raises the alarming possibility of transmission of animal prions through corneal abrasions.

Highlights

  • Iron is an essential catalyst for vital biochemical reactions because of the ease with which it can donate and accept electrons

  • The eye is protected further from fluctuations in systemic iron by the outer and inner blood-retinal barriers comprised of retinal pigment epithelial cells and capillary endothelial cells respectively, and the blood aqueous barrier formed by epithelial cells of the ciliary body (CB)

  • Proteome analysis of the aqueous humor (AH) suggests active synthesis and transport of several proteins by the ciliary epithelium, including proteins involved in iron transport (Bertazolli-Filho et al, 2003, 2006; Chowdhury et al, 2010)

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Summary

Introduction

Iron is an essential catalyst for vital biochemical reactions because of the ease with which it can donate and accept electrons. The eye is protected further from fluctuations in systemic iron by the outer and inner blood-retinal barriers comprised of retinal pigment epithelial cells and capillary endothelial cells respectively, and the blood aqueous barrier formed by epithelial cells of the ciliary body (CB). The inner pigmented layer is continuous with retinal pigment epithelial cells of the outer retina. The outer layer is non-pigmented, faces the AH, and is continuous with neural retina. Non-pigmented epithelial (NPE) cells are polarized and form the functional blood-aqueous barrier. The apical surface of pigmented epithelium (PE) and NPE is juxtaposed, and separated by gap junctions to form a syncytium. This results in the coupling of PE and NPE cells in trans-epithelial transport. Proteome analysis of the AH suggests active synthesis and transport of several proteins by the ciliary epithelium, including proteins involved in iron transport (Bertazolli-Filho et al, 2003, 2006; Chowdhury et al, 2010)

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