Abstract

The neuroglia of CNS are in intimate contact with the surfaces of neurons and are thus strategically placed for the delivery of secreted therapeutic agents. However, in vivo delivery of transforming agents such as DNA or liposomes to these cells is problematic because of the extremely narrow intracellular space of the CNS. Recent evidence from retroviral marking experiments indicates that both astrocytes and oligodendrocytes or their progenitors migrate over substantial distances during development; thus, progenitors isolated and transformed in vitro, or strategic populations transformed locally in vivo, might by subsequent migration colonize widely. This product will test the hypothesis that migrating neuroglia can deliver therapeutic agents. In the first place, the extent and patterns of migration of transgenically marked populations of astrocytes and microglia transplanted into murine CNS at various pre- and postnatal stages. These data, along with similar information on native oligodendrocytes currently being generated in an ongoing project, will at once reveal principles of organization of normal neural development and will underpin attempts to use these populations, after genetic modification, as delivery vehicles for secreted therapeutic agents. In addition, we have recently discovered that immature neuroglia transplanted into the cerebral ventricles will migrate into the brain parenchyma. we will determine the identity of the migrating neuroglia and their eventual fate to determine if this route of administration might be effective for the delivery of genetically modified neuroglia. The second phase of this project will explore the utility of implanted neuroglia as in vivo secretors of engineered proteins, by transplanting transgenically marked cells into murine lysosomal storage disease models to analyze the effect of these disorders on neuroglial cell migration. Finally, neuroglial cells secreting modified, putative therapeutic lysosomal proteins will be obtained from transgenic mouse lines or by transfection of neuroglia from normal mice. These cells will be implanted in the same lysosomal storage disease models in an attempt to develop a cell-transplant based model for lysosomal storage disease therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD032654-05
Application #
6108772
Study Section
Project Start
1998-12-01
Project End
2000-11-30
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
5
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Mount Sinai School of Medicine
Department
Type
DUNS #
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Miranda, S R; Erlich, S; Friedrich Jr, V L et al. (2000) Hematopoietic stem cell gene therapy leads to marked visceral organ improvements and a delayed onset of neurological abnormalities in the acid sphingomyelinase deficient mouse model of Niemann-Pick disease. Gene Ther 7:1768-76
Schuchman, E H; Erlich, S; Miranda, S R et al. (2000) Fluorescence-based selection of gene-corrected hematopoietic stem and progenitor cells based on acid sphingomyelinase expression. Methods Enzymol 312:330-8
Miranda, S R; He, X; Simonaro, C M et al. (2000) Infusion of recombinant human acid sphingomyelinase into niemann-pick disease mice leads to visceral, but not neurological, correction of the pathophysiology. FASEB J 14:1988-95
Erlich, S; Miranda, S R; Visser, J W et al. (1999) Fluorescence-based selection of gene-corrected hematopoietic stem and progenitor cells from acid sphingomyelinase-deficient mice: implications for Niemann-Pick disease gene therapy and the development of improved stem cell gene transfer procedures. Blood 93:80-6
Miranda, S R; Erlich, S; Friedrich Jr, V L et al. (1998) Biochemical, pathological, and clinical response to transplantation of normal bone marrow cells into acid sphingomyelinase-deficient mice. Transplantation 65:884-92
Chen, F W; Davies, J P; Ioannou, Y A (1998) Differential gene expression in apoptosis: identification of ribosomal protein 23K, a cell proliferation inhibitor. Mol Genet Metab 64:271-82
Schuchman, E H; Miranda, S R (1997) Niemann-Pick disease: mutation update, genotype/phenotype correlations, and prospects for genetic testing. Genet Test 1:13-9
Davies, J P; Cotter, P D; Ioannou, Y A (1997) Cloning and mapping of human Rab7 and Rab9 cDNA sequences and identification of a Rab9 pseudogene. Genomics 41:131-4
Miranda, S R; Erlich, S; Visser, J W et al. (1997) Bone marrow transplantation in acid sphingomyelinase-deficient mice: engraftment and cell migration into the brain as a function of radiation, age, and phenotype. Blood 90:444-52
Ioannou, Y A; Chen, F W (1996) Quantitation of DNA fragmentation in apoptosis. Nucleic Acids Res 24:992-3

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