Advances in stem cell therapy for glaucoma

Keith Martin

Potential treatment strategies

Theoretically, the most direct stem cell based treatment for glaucoma would involve stimulation of endogenous retinal repair mechanisms. In fish and amphibians, retinal regeneration is an automatic process that proceeds via differentiation of ocular stem cells located in the ciliary marginal zone. In adult mammals, however, retinal regeneration after injury or in neurodegenerative disease does not occur. While mammalian retinal progenitor cells have been identified in vitro, they appear to remain quiescent in vivo. Within the adult mammalian CNS, neurogenesis is limited to discrete regions such as the hippocampus and elsewhere the environment is notoriously resistant to the generation and integration of new neurons. Techniques to enhance neuronal repair in the adult human eye remain at an early stage of development.

Alternatively, degenerated retinal neurons could be replaced by transplanting suitable precursor cells. It has been demonstrated that neural precursor cells derived from embryonic stem cells, when transplanted into the eye, can migrate into the retina and express markers of mature retinal neurons.¹ In addition, retinal progenitor cells derived from neonatal animals have been shown to achieve retinal integration, to exhibit photoreceptor differentiation and to provide some functional benefit to animals with retinal dystrophy.² Transplanted foetal-derived hippocampal progenitors also demonstrate the ability to localize to the retinal ganglion cell layer, from where they may extend neurites into the inner plexiform layer and towards the optic nerve head.³ Human adult retina derived Muller stem cells can survive in the glaucomatous rat eye and a small proportion show signs of integration when the inhibitory host retinal extracellular matrix is modulated with chondroitinase.⁴ However, the migration and incorporation of transplanted cells is difficult to achieve in the adult mammalian retina. Furthermore, the challenge of glaucomatous retinal regeneration does not end at the optic disc. In order to achieve complete functional repair in glaucoma, transplanted cells would not only need to integrate into the existing retinal circuitry but re-establish functional connections with target neurons in the brain with precise regeneration of the retinotopic map. New axons would also require myelination to allow signal conduction at the appropriate velocity. Obviously, significant progress must be made before stem cell therapy can be used to repair the visual pathway so comprehensively. However, it is possible that the survival and partial integration of transplanted cells within the retina could provide alternative benefits by enhancing the survival and function of host RGCs. Recent research suggests that transplantation of stem cells within the CNS can provide neuroprotection to surviving neurons near the graft site.⁵ Transplanted cells have also demonstrated an ability to modulate immune cell behaviour to reduce tissue damage.⁶ We have demonstrated that transplantation of oligodendrocyte precursor cells can protect host retinal ganglion cells in a rat model of glaucoma.⁷

Barriers to progress

References

1.  Banin E, Obolensky A, Idelson M, et al. Retinal incorporation and differentiation of neural precursors derived from human embryonic stem cells. Stem Cells 2006; 24: 246-257.
2.  MacLaren RE, Pearson RA, MacNeil A, et al. Retinal repair by transplantation of photoreceptor precursors. Nature 2006; 444: 203-207.
3.  Young MJ, Ray J, Whiteley SJ, Klassen H, Gage FH. Neuronal differentiation and morphological integration of hippocampal progenitor cells transplanted to the retina of immature and mature dystrophic rats. Mol Cell Neurosci 2000; 16: 197-205.
4.  Bull ND, Limb GA, Martin KR. Human Muller stem cell (MIO-M1) trans plantation in a rat model of glaucoma: survival, differentiation, and integration. Invest Ophthalmol Vis Sci 2008; 49: 3449-3456.
5.  Meyer JS, Katz ML, Maruniak JA, Kirk MD. Embryonic stem cell-derived neural progenitors incorporate into degenerating retina and enhance survival of host photoreceptors. Stem Cells 2006; 24: 274-283.
6.  Pluchino S, Zanotti L, Rossi B, et al. Neurosphere-derived multipotent precursors promote neuroprotection by an immunomodulatory mechanism. Nature 2005; 436: 266-271.
7.  Bull ND, Irvine KA, Franklin RJ, Martin KR. Transplanted oligodendrocyte precursor cells reduce neurodegeneration in a model of glaucoma. Invest Ophthalmol Vis Sci 2009; 50: 4244-4253.