Transient Immunosuppression Stops Rejection of Virus-Transduced Enhanced Green Fluorescent Protein in Rabbit Retina

Doi, Kentaro; Kong, Jian; Hargitai, J.; Goff, Stephen P.; Gouras, Peter

doi:10.1128/jvi.78.20.11327-11333.2004

Cited by 12 publications

(9 citation statements)

References 21 publications

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“…Genetic similarity, generally, obviates immunosuppression under these conditions. It has been demonstrated recently, however, that expression of foreign proteins within CNS cells transduced in vivo can elicit immunemediated rejection, which is prevented by immunosuppression (Doi et al, 2004). This suggests that foreign proteins expressed within the CNS can be appropriately presented to host immune cells and recognized as nonself, resulting in immune-mediated rejection.…”

mentioning

confidence: 99%

Labeled Schwann cell transplantation: Cell loss, host Schwann cell replacement, and strategies to enhance survival

Hill

Moon

Wood

et al. 2005

Glia

143

115

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Although transplanted Schwann cells (SCs) can promote axon regeneration and remyelination and improve recovery in models of spinal cord injury, little is known about their survival and how they interact with host tissue. Using labeled SCs from transgenic rats expressing human placental alkaline phosphatase (PLAP), SC survival in a spinal cord contusion lesion was assessed. Few PLAP SCs survived at 2 weeks after acute transplantation. They died early due to necrosis and apoptosis. Delaying transplantation until 7 days after injury improved survival. A second wave of cell death occurred after surviving cells had integrated into the spinal cord. Survival of PLAP SCs was enhanced by immunosuppression with cyclosporin; delayed transplantation in conjunction with immunosuppression resulted in the best survival. In all cases, transplantation of SCs resulted in extensive infiltration of endogenous p75+ cells into the injury site, suggesting that endogenous SCs may play an important role in the repair observed after SC transplantation.

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confidence: 99%

Labeled Schwann cell transplantation: Cell loss, host Schwann cell replacement, and strategies to enhance survival

Hill

Moon

Wood

et al. 2005

Glia

143

115

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“…Embryonic or neonatal donor tissue is not an ideal repair strategy due to supply limitations. Both tissue and cell transplantation are subject to immune response, although graft survival may be improved by intravitreal injections or sustained release of immunosuppressive drugs [125,126]. Progenitor cells possess low immunogenicity [127] and can be adult derived and cultured for extended time allowing for a continued cell source.…”

Section: Cell Transplant Conclusionmentioning

confidence: 99%

A tissue-engineered approach towards retinal repair: Scaffolds for cell transplantation to the subretinal space

Hynes

Lavik

2010

Graefes Arch Clin Exp Ophthalmol

159

135

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“…[76] In a rabbit model, termination of LV transduced GFP expression in RPE was also associated with inflammation but one month of systemic immunosuppression, starting the day of injection, prevented loss of GFP expression. [28] In monkeys, FIVmediated transgene expression in the TM lasted more than 1 year after a single intracameral injection (Poeschla EM, Loewen N, Rasmussen C, et al Transduction of Nonhuman Primate Trabecular Meshwork With Lentiviral Vectors. ARVO Abnr 2696, 2006).…”

Section: Viral Delivery Systemsmentioning

confidence: 99%

Gene Therapy Targeting Glaucoma: Where Are We?

Liu

Rasmussen

Gabelt

et al. 2009

Survey of Ophthalmology

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In a chronic disease such as glaucoma, a therapy that provides a long lasting local effect, with minimal systemic side effects, while circumventing the issue of patient compliance, is very attractive. The field of gene therapy is growing rapidly and ocular applications are expanding. Our understanding of the molecular pathogenesis of glaucoma is leading to greater specificity in ocular tissue targeting. Improvements in gene delivery techniques, refinement of vector construction methods, and development of better animal models combine to bring this potential therapy closer to reality.

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Transient Immunosuppression Stops Rejection of Virus-Transduced Enhanced Green Fluorescent Protein in Rabbit Retina

Cited by 12 publications

References 21 publications

Labeled Schwann cell transplantation: Cell loss, host Schwann cell replacement, and strategies to enhance survival

Labeled Schwann cell transplantation: Cell loss, host Schwann cell replacement, and strategies to enhance survival

A tissue-engineered approach towards retinal repair: Scaffolds for cell transplantation to the subretinal space

Gene Therapy Targeting Glaucoma: Where Are We?

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