Abstract

Efficient gene transfer and high-level expression are the major goals of any gene therapy strategy. We have selected retroviral insertion of the ferrochelatase gene (FC) in erythropoietic protoporphyria (EPP) in hematopoietic stem cells as our model system. The ferrochelatase gene and cDNA have previously been described, and are amenable to PCR and manipulation leading to the development of gene therapy for EPP. The molecular basis of EPP is firmly established, in that a large number of mutations in FC have been described which are causally related to the pathoetiology of EPP. Cultured EPP fibroblasts can be transduced with recombinant FC, and enzyme levels are restored to normal, demonstrating in vivo phenotypic reversion. Thus, demonstration of in vitro phenotypic reversion would represent the critical step in a preclinical study aimed at applying gene therapy to EPP. The relatively small FC cDNA is only 1.6 kb in size, and can therefore be easily cloned and manipulated in insert-size restricted retroviral vectors. Second, the gene product itself is labile, and is ubiquitously expressed in all tissues examined, thereby obviating the need for targeted cell-type specific gene expression. Third, techniques for selection, enrichment and transduction of hematopoietic stem cells are already well-established. Fourth, phenotypic reversion of EPP can be monitored in vivo not only by levels of expression of the FC gene, but importantly, by demonstrating the functionality of the gene product by an FC enzyme activity assay. Fifth, partial gene expression may be sufficient for phenotypic reversion, since we know from some clinically unaffected EPP heterozygotes that achieving 100% gene replacement efficiency may be unnecessary, as many individuals with significantly reduced enzyme levels are asymptomatic. Collectively, these features underscore the feasibility of developing gene therapy for EPP, which could potentially lead to therapeutic strategies for the other forms of porphyria, as well.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Center Core Grants (P30)
Project #
1P30AR044535-01
Application #
6235865
Study Section
Project Start
1997-07-20
Project End
1998-06-30
Budget Start
1996-10-01
Budget End
1997-09-30
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Shen, Yao; Stanislauskas, Milda; Li, Gen et al. (2017) Epigenetic and genetic dissections of UV-induced global gene dysregulation in skin cells through multi-omics analyses. Sci Rep 7:42646
Mathew, Grinu; Hannan, Abdul; Hertzler-Schaefer, Kristina et al. (2016) Targeting of Ras-mediated FGF signaling suppresses Pten-deficient skin tumor. Proc Natl Acad Sci U S A 113:13156-13161
Shen, Yao; Kim, Arianna L; Du, Rong et al. (2016) Transcriptome Analysis Identifies the Dysregulation of Ultraviolet Target Genes in Human Skin Cancers. PLoS One 11:e0163054
Dai, Zhenpeng; Xing, Luzhou; Cerise, Jane et al. (2016) CXCR3 Blockade Inhibits T Cell Migration into the Skin and Prevents Development of Alopecia Areata. J Immunol 197:1089-99
Abaci, Hasan E; Guo, Zongyou; Coffman, Abigail et al. (2016) Human Skin Constructs with Spatially Controlled Vasculature Using Primary and iPSC-Derived Endothelial Cells. Adv Healthc Mater 5:1800-7
Dainichi, Teruki; Hayden, Matthew S; Park, Sung-Gyoo et al. (2016) PDK1 Is a Regulator of Epidermal Differentiation that Activates and Organizes Asymmetric Cell Division. Cell Rep 15:1615-23
Johnson, Dylan; Mathur, Mohit C; Kobayashi, Tomoyoshi et al. (2016) The Cardiomyopathy Mutation, R146G Troponin I, Stabilizes the Intermediate ""C"" State of Regulated Actin under High- and Low-Free Ca(2+) Conditions. Biochemistry 55:4533-40
Shinkuma, Satoru; Guo, Zongyou; Christiano, Angela M (2016) Site-specific genome editing for correction of induced pluripotent stem cells derived from dominant dystrophic epidermolysis bullosa. Proc Natl Acad Sci U S A 113:5676-81
Kim, Arianna L; Back, Jung Ho; Zhu, Yucui et al. (2016) AKT1 Activation is Obligatory for Spontaneous BCC Tumor Growth in a Murine Model that Mimics Some Features of Basal Cell Nevus Syndrome. Cancer Prev Res (Phila) 9:794-802
Sun, Xiaoyun; Kim, Arianna; Nakatani, Masashi et al. (2016) Distinctive molecular responses to ultraviolet radiation between keratinocytes and melanocytes. Exp Dermatol 25:708-13

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