Abstract

Retinal transplantation represents a rational approach for the treatment of blinding diseases of the retina. However, there are significant obstacles that must first be overcome before one can contemplate such interventions in a clinical setting. Among the most daunting barriers to successful grafting of new cells to the retina are 1) the capacity of the immune system to recognize and destroy grafted tissue placed into the eye; and 2) the ability of grafted tissue to survive, differentiate, and form functional connections with the host neuroretina. We have recently made new observations regarding 1) the role of microglia in the immunogenicity of retinal transplants; and 2) the immunogenicity of RPE cells. There have also been significant advances in the field of neural stem cell biology. We have used these immature, multipotent cells to overcome one fundamental barrier to successful retinal transplantation, the achievement of morphological integration of grafted tissue in the mature, diseased mammalian retina. In this application, we propose a series of experiments that will address what we consider to be the two key issues in the field of retinal transplantation; 1) immunobiology of retinal grafts; and 2) integration of grafted tissue with the host retina. We will 1) analyze the role of microglia in the immunogenicity and vulnerability to rejection of neuronal retinal transplants placed orthotopically and heterotopically; 2) analyze the immunogenicity of RPE cells as grafts and their vulnerability to rejection when placed orthotopically and heterotopically; 3) analyze the immunogenicity and vulnerability to rejection of CNS derived stem cells grafted orthotopically and heterotopically; and 4) study the fate of retinal stem cells implanted intraocularly. The anticipated results of these experiments will allow us to develop strategies aimed at producing retinal transplants that survive and form functional connections in the eyes of rodents with retinal dystrophies. We believe the demonstration of functionally integrated grafts, which also survive for long periods of time in an allogeneic setting, are vital and necessary prerequisites to further studies in higher animals. While all the studies proposed in this application involve the use of rodents, the knowledge gained will have relevance to humans, and will offer insight that might someday allow us to approach retinal transplantation in patients with blinding diseases of the retina.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
2R01EY009595-11
Application #
6330820
Study Section
Special Emphasis Panel (ZRG1-VISC (02))
Program Officer
Dudley, Peter A
Project Start
1992-05-01
Project End
2004-06-30
Budget Start
2001-07-01
Budget End
2002-06-30
Support Year
11
Fiscal Year
2001
Total Cost
$348,000
Indirect Cost

  Institution

Name
Schepens Eye Research Institute
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02114

  Publications

Klassen, Henry; Warfvinge, Karin; Schwartz, Philip H et al. (2008) Isolation of progenitor cells from GFP-transgenic pigs and transplantation to the retina of allorecipients. Cloning Stem Cells 10:391-402
Klassen, Henry; Schwartz, Philip H; Ziaeian, Boback et al. (2007) Neural precursors isolated from the developing cat brain show retinal integration following transplantation to the retina of the dystrophic cat. Vet Ophthalmol 10:245-53
Klassen, Henry; Kiilgaard, Jens Folke; Zahir, Tasneem et al. (2007) Progenitor cells from the porcine neural retina express photoreceptor markers after transplantation to the subretinal space of allorecipients. Stem Cells 25:1222-30
Schwartz, Philip H; Nethercott, Hubert; Kirov, Ivan I et al. (2005) Expression of neurodevelopmental markers by cultured porcine neural precursor cells. Stem Cells 23:1286-94
Zamiri, Parisa; Masli, Sharmila; Kitaichi, Nobuyoshi et al. (2005) Thrombospondin plays a vital role in the immune privilege of the eye. Invest Ophthalmol Vis Sci 46:908-19
Zahir, Tasneem; Klassen, Henry; Young, Michael J (2005) Effects of ciliary neurotrophic factor on differentiation of late retinal progenitor cells. Stem Cells 23:424-32
Klassen, Henry; Ziaeian, Boback; Kirov, Ivan I et al. (2004) Isolation of retinal progenitor cells from post-mortem human tissue and comparison with autologous brain progenitors. J Neurosci Res 77:334-43
Klassen, Henry J; Ng, Tat Fong; Kurimoto, Yasuo et al. (2004) Multipotent retinal progenitors express developmental markers, differentiate into retinal neurons, and preserve light-mediated behavior. Invest Ophthalmol Vis Sci 45:4167-73
Zamiri, Parisa; Zhang, Qiang; Streilein, J Wayne (2004) Vulnerability of allogeneic retinal pigment epithelium to immune T-cell-mediated damage in vivo and in vitro. Invest Ophthalmol Vis Sci 45:177-84
Klassen, Henry J; Imfeld, Karen L; Kirov, Ivan I et al. (2003) Expression of cytokines by multipotent neural progenitor cells. Cytokine 22:101-6

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