Functional properties of retinal Müller cells following transplantation to the anterior eye chamber.

Two types of glial cells occur in the retina, Müller cells and astrocytes. These cells share several structural features such as extending endfeet onto blood vessels of the retina. Retinal vessels express a tight blood-retinal barrier which is comparable to the blood-brain barrier (BBB) of the CNS. While astrocytes have been implicated in the induction of the BBB, the role of Müller cells in the blood-retinal barrier is unknown. To determine if Müller cells are capable of influencing vascular permeability, we have prepared Müller cells that are free of astrocytes and transplanted them to a peripheral target, the anterior eye chamber. Müller cells were identified 2 weeks to 3 months after injection and were predominantly localized within the connective tissue of the ciliary body. The Müller cells occurred as dense clusters of cells closely associated with ciliary blood vessels. The ciliary vessels adjacent to Müller cells were freely permeable to circulating horseradish peroxidase (HRP), suggesting that Müller cells did not induce tight barrier properties from these leaky peripheral vessels. In contrast, cortical astrocytes injected into the anterior eye chamber preferentially formed a monolayer on the anterior surface of the iris, a region known to contain blood vessels that are impermeable to circulating tracers (e.g., Raviola, Exp Eye Res [Suppl] 25:27, 1977). Müller cells were rarely associated with the iris and the few cells that were present were located deep within the iris stroma rather than on the surface. The behaviour of guinea pig Müller cells transplanted to the anterior eye chamber contrasts sharply with that of cortical astrocytes in terms of: 1) the ocular compartment to which Müller cells migrate; 2) the tissue invasiveness of the cells; and 3) the degree of permeability of blood vessels adjacent to transplanted cells. The results of this study emphasize the functional distinctness of the two types of retinal glia and suggest that Müller cells from guinea pig retina may not be active in modifying the permeability properties of peripheral blood vessels, a function that has been suggested for astrocytes.