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Development of a Stem Cell Therapy for Glaucoma of Leber’s congenital amaurosis. 8 The grafted cells integrated into the outer nuclear layer and exhibited morphology similar to native photoreceptors. Recently, a first clinical trial on hESC-derived retinal pigment epithelium (RPE) cell transplantation in patients with Stargardt’s macular dystrophy and atrophic age-related macular degeneration showed an encouraging result. 9 Despite the fact that one patient with Stargardt’s macular dystrophy developed severe vitreous cavity inflammation consistent with acute postoperative endophthalmitis 4 days after the surgery and one developed vitreous inflammation, no rejection or tumor formation was observed in any of the patients. Half of the patients appeared to have improved visual acuity 22 months after subretinal injection of hESC-derived RPEs. The finding suggests that cell-replacement therapy with hESC-derived cells can be a promising treatment modality for retinal degeneration. Cellular senescence of the TM 27 and decreases in numbers of TM-cells with aging 13 have been reported and are speculated to contribute to the pathophysiology of glaucoma. 2 Stem cell replacement therapy has also been shown to benefit ocular surface diseases. Corneal diseases or wound healing can be complicated by opacification of the transparent epithelium. Although transplantation of donor corneas is commonly practiced in clinics, increasing shortage of corneal donors and the risk for immune rejection present significant challenges. Regular turnover and repair of corneal epithelial cells occurs through limbal SCs, 10,11 and transplantation of limbal SCs thus has brought opportunities for reconstructing the ocular surface and reversing vision loss. Successful restoration of a transparent cornea with differentiated epithelial cells has been observed in animal studies of undifferentiated ESC transplantation. 12 Emerging evidence indicates that application of cultivated Adult TM SCs can be differentiated into cells characteristic of corneal epithelium, phagocytotic TM cells, and retinal neurons in vitro. 36 Phagocytosis is an important function of TM cells. Moreover, transplanted TM SCs home to the TM following injection into the healthy mouse anterior chambers. 15 Human iPSC-derived TM cells also resemble native hTM, with similar morphology and the ability of phagocytosis. 35 Whereas, transplanted bone marrow-derived MSCs primarily exert their benefits through a paracrine effect that recruits progenitor cells to promote TM regeneration. 14 Injection of MSCs into the anterior chamber of rats SCs for corneal surface reconstruction is coming of age. Stem Cell Treatment for Glaucoma Development of stem cell therapies for glaucoma has been focused on the replacement of two cell types: cells of the trabecular meshwork (TM) and RGCs. TM cells decrease with age, 13 and it is evident that there is more cell loss in the TM of glaucomatous eyes compared with age-matched normal eyes. 2 A recent study in an animal model of glaucoma suggests that transplantation of SCs to the TM lowers IOP through TM cell recovery, enhanced ocular outflow, and progenitor cell recruitment. 14 In an independent study, injection of TM SCs or fibroblasts into normal C57BL/6 mice does not alter IOP compared with noninjected controls, 15 further supporting the therapeutic potential for TM stem cell transplantation without impacting TM’s normal function. Replacing damaged RGCs with SCs faces several obstacles, but evidence suggests that SCs may release trophic factors 16–18 and work to the benefit of existing RGCs through a neuroprotective mechanism without requiring optic nerve reformation and functional integration. In this review, research attempts trying to replace both TM and RGCs, the two cell types mainly affected by glaucoma, will be discussed. Trabecular Meshwork Cells Derived from Stem Cells Disruption of the TM, 19 where aqueous humor is drained, is thought to cause elevated IOP, leading to glaucoma. These disruptions are reflected in both cell motility and endothelial function, which may include changes in cell shape, size, and permeability, and accumulation of damaged and cross-linked proteins with malfunctioning proteolytic cellular systems. 20–25 Increases in oxidative stress also induces mitochondrial damage and trigger cell apoptosis. Treatment of dysfunctional TM thus may present a viable therapy. The aqueous humor circulates from the ciliary body through the anterior chamber to the TM. The primary function of TM is to maintain the aqueous flow and remove foreign objects through phagocytosis. 26,27 U S Oph th a l mic Review Accumulating evidence suggests that stem-like cells reside in the transitional area between the peripheral corneal and TM. 28 SCs, including adult TM SCs and MSCs, are found in the human TM (hTM). 14,15 Stem-like cells in the TM were first discovered by Raviola in the early 80s, 29 which were later shown to possess stem-like properties and express distinct biomarkers. 30–33 Interestingly, MSCs derived from the TM express TM- specific markers, suggesting that they are TM-specific progenitors, forming a reservoir for TM repairs. 34 A recent report suggests that TM cells may also be derived from iPSCs. 35 with laser-induced glaucoma significantly decreased IOP and improved the histology of the angle structure without observing permanently integrated MSCs in the host tissue. This paracrine effect of MSCs was confirmed using the medium conditioned by cultured MSCs. To date, proof of concept studies for a stem cell therapy for TM repair have been carried out in animals. Importantly, transplantation of iPS cell-derived TM cells into the anterior segments reestablished IOP homeostatic function in perfused human outflow pathway organ cultures. 37 Together, these studies establish the conceptual feasibility of a cell-replacement approach for restoring IOP regulatory function, supporting a potential benefit for human patients with open-angle glaucoma. Cell Therapy for Treating RGC Damage The neuroretina, specifically RGCs, is irreversibly damaged in glaucoma. Thus, neuroprotection focused on improving neuron survival and preventing progressive RGC damage is critical. Multiple studies have reported beneficial effects on the survival of injured RGCs and improved visual function in animal models of optic neuropathy, 38–42 suggesting the nature of neuroprotective effects by transplanted SCs. The beneficial effects could also be seen by injecting secretome or conditioned medium of SCs, 43,44 associated with the production of platelet-derived growth factors 43 and extracellular matrix proteins. 44,45 Embryonic mouse neural SCs modified to secrete ciliary neurotrophic factor were shown not only attenuating RGC axon loss but stimulating long-distance axonal regrowth. 46 Therefore, the stem cell approach is appealing because it presents a source of sustained production of neuroprotective and growth-stimulating factors. Ideally, beyond neuroprotection, a more sophisticated use of stem cell technology could be applied to replace RGCs that have been lost and reverse vision loss. However, this approach is faced with several obstacles. Present protocols for pluripotent stem cell differentiation often generate a heterogeneous population of neurons and glial cells. 47–51 Moreover, differentiated neurons, in contrast to early-stage SCs, have limited ability 53