CEP290 gene transfer rescues Leber congenital amaurosis cellular phenotype

Burnight, Erin R; Wiley, Luke A; Drack, Arlene V.; Braun, Terry A.; Anfinson, Kristin R.; Kaalberg, Emily E.; Halder, Jennifer A; Affatigato, Louisa M.; Mullins, Robert F.; Stone, Edwin M.; Tucker, Budd A.

doi:10.1038/gt.2014.39

Cited by 115 publications

(120 citation statements)

References 48 publications

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“…CEP290 is a gene frequently mutated in several ciliopathies and LCA (6). CEP290 gene augmentation therapy using viral vectors has been shown to ameliorate LCA-related phenotypes in human cell and mouse models (7,8). Oligonucleotide-mediated splicing correction has also been shown to rescue LCA phenotypes in the induced pluripotent stem cell-derived optic cups of patients harboring a CEP290 intronic mutation (9).…”

Section: Introductionmentioning

confidence: 99%

Eupatilin rescues ciliary transition zone defects to ameliorate ciliopathy-related phenotypes

Kim¹,

Kim²,

Jung³

et al. 2018

Journal of Clinical Investigation

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Section: Introductionmentioning

confidence: 99%

Eupatilin rescues ciliary transition zone defects to ameliorate ciliopathy-related phenotypes

Kim¹,

Kim²,

Jung³

et al. 2018

Journal of Clinical Investigation

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“…[1][2][3][4] Gene therapy started from a concept of correcting an abnormal gene by delivering a desirable therapeutic transgene (i.e., DNA), 5 and has recently evolved to interfere with target biological activities at a translational level by delivering small nucleic acids (e.g., siRNA and antisense ODN). 6,7 In order to address the clinical challenges associated with using viral vectors (e.g., immunogenicity, onco/tumorigenicity, and inefficient and cumbersome preparation), 8,9 developing nonviral vectors that are as efficient as viral counterparts with improved safety measures has been of great interest.…”

Section: Introductionmentioning

confidence: 99%

Mixing-sequence-dependent nucleic acid complexation and gene transfer efficiency by polyethylenimine

et al. 2015

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Polyplexes, complexed nucleic acids by cationic polymers, are the most common forms of nonviral gene delivery vectors. In contrast to a great deal of efforts in synthesizing novel cationic polymers and exploring their extracellular and intracellular delivery pathways, polyplex preparation methods of mixing nucleic acids and cationic polymers are often overlooked. In this study, the mixing sequence, that is adding nucleic acids to polymers or vice versa, was found to greatly affect complexation of both plasmid DNA and siRNA, polyplexes' size, and polyplexes' surface charge, which all collaboratively affected the transfection efficiency and cytotoxicity. Adding polyethylenimine (PEI), the most conventionally used standard in nonviral gene delivery, to plasmid DNA and siRNA resulted in larger polyplexes, higher gene expression and silencing, but higher cytotoxicity than polyplexes prepared in the reverse order. Based on the experimental results, the authors developed a model that gradual addition of cationic polymers (e.g., PEI) to nucleic acids (e.g., plasmid DNA and siRNA) incorporates more copies of nucleic acids in larger polyplexes in a smaller number, results in higher gene expression and silencing levels in transfected cells, and generates higher cytotoxicity by leaving more free polymers upon complete mixing than the other mixing sequence. The proposed model can be explored using a broad range of cationic polymers and nucleic acids, and provide insightful information about how to prepare polyplexed nonviral vectors for efficient and safe gene delivery.

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“…61 iPSC-derived photoreceptor precursor cells carrying an USH2A mutation showed increased ER stress due to misfolding of the protein. 61 iPSCderived photoreceptor precursors, this time from a patient with Leber congenital amaurosis caused by mutation in CEP290, have been used to test lentiviral vectors for gene replacement therapy 62 ; viral transduction improved the ciliogenesis defect in cells from affected individuals.…”

Section: Ipsc Retinal Disease Modelingmentioning

confidence: 99%

Induced Pluripotent Stem Cell Therapies for Degenerative Disease of the Outer Retina: Disease Modeling and Cell Replacement

Foggia

Makwana

Ali³

et al. 2016

Journal of Ocular Pharmacology and Therapeutics

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Stem cell therapies are being explored as potential treatments for retinal disease. How to replace neurons in a degenerated retina presents a continued challenge for the regenerative medicine field that, if achieved, could restore sight. The major issues are: (i) the source and availability of donor cells for transplantation; (ii) the differentiation of stem cells into the required retinal cells; and (iii) the delivery, integration, functionality, and survival of new cells in the host neural network. This review considers the use of induced pluripotent stem cells (iPSC), currently under intense investigation, as a platform for cell transplantation therapy. Moreover, patientspecific iPSC are being developed for autologous cell transplantation and as a tool for modeling specific retinal diseases, testing gene therapies, and drug screening.

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CEP290 gene transfer rescues Leber congenital amaurosis cellular phenotype

Cited by 115 publications

References 48 publications

Eupatilin rescues ciliary transition zone defects to ameliorate ciliopathy-related phenotypes

Eupatilin rescues ciliary transition zone defects to ameliorate ciliopathy-related phenotypes

Mixing-sequence-dependent nucleic acid complexation and gene transfer efficiency by polyethylenimine

Induced Pluripotent Stem Cell Therapies for Degenerative Disease of the Outer Retina: Disease Modeling and Cell Replacement

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