Abstract

Progressive childhood diseases should be treated before pathological sequelae are evident. A technically promising but underdeveloped approach experimentally and clinically is in utero transplantation. Two major causes for unsuccessful human in utero therapy were identified by animal studies. They are micro- rather than macro-chimerism following congenic and allogeneic transfers and allogeneic donor cell rejection initiated by unexpected and inexplicable immune complications. It is critical that we understand the mechanisms behind these failures and develop alternative approaches to correct them. This is the goal of our current proposal. We investigate stem cell biology and curative interventions in Mucopolysaccharidosis type VII (MPS VII) mice, a model that mimics human lysosomal storage diseases. MPS VII mice lack the enzyme beta glucuronidase (GUSB). This allows us to track and enumerate GUSB+ donor cells by histochemistry and confirm our results by flow cytometry, biochemistry, and pathogenesis. Disease symptoms are ameliorated by enzyme replacement. We compared repopulation in genetically myeloablated and non-ablated MPS VII fetal recipients of congenic fetal GUSB+ hematopoietic cells. Results indicate that the donor cells do not have a selective advantage as previously hypothesized in the rapidly growing nonablated fetuses. Surprisingly, donor cells do amplify modestly between birth and one week of age and are maintained at a low percentage long term. Donor cells undergo rapid proliferation within 24 hours in the genetically myeloablated fetus and increase thereafter until they completely repopulate the host. We predict that donor cell amplification is directly linked to levels of stem cell implantation. Following allogeneic transfers, there are reasons to believe that the dam and fetus supply immunologically competent cells to one another and that allogeneic donor cell expansion after birth occurs in a hostile environment. We hypothesize that significant allogeneic donor cell implantation and expansion can be effected in utero without serious immune consequences.
Our aims are to: Determine if donor stem cell implantation levels in utero affect subsequent stem and differentiated cell amplification; Identify procedures that increase corrective donor cells in the fetus; Define the role of dam and fetal immune response in allogeneic in utero transplantation; and Block immune responses to allogeneic cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK049525-09
Application #
6687878
Study Section
Hematology Subcommittee 2 (HEM)
Program Officer
Mckeon, Catherine T
Project Start
1994-09-30
Project End
2007-07-31
Budget Start
2003-09-01
Budget End
2004-07-31
Support Year
9
Fiscal Year
2003
Total Cost
$383,997
Indirect Cost

  Institution

Name
Jackson Laboratory
Department
Type
DUNS #
042140483
City
Bar Harbor
State
ME
Country
United States
Zip Code
04609

  Publications

Ohgami, Robert S; Campagna, Dean R; Antiochos, Brendan et al. (2005) nm1054: a spontaneous, recessive, hypochromic, microcytic anemia mutation in the mouse. Blood 106:3625-31
Vogler, Carole; Levy, Beth; Galvin, Nancy et al. (2005) Early onset of lysosomal storage disease in a murine model of mucopolysaccharidosis type VII: undegraded substrate accumulates in many tissues in the fetus and very young MPS VII mouse. Pediatr Dev Pathol 8:453-62
Schuldt, A J T; Hampton, T J; Chu, V et al. (2004) Electrocardiographic and other cardiac anomalies in beta-glucuronidase-null mice corrected by nonablative neonatal marrow transplantation. Proc Natl Acad Sci U S A 101:603-8
Barker, Jane E; Schuldt, Adam J T; Lessard, Mark L et al. (2003) Donor cell expansion is delayed following nonablative in utero transplantation to treat murine mucopolysaccharidosis type VII. Exp Hematol 31:1112-8
Barker, J E; Schuldt, A J T; Lessard, M D et al. (2003) Donor cell replacement in mice transplanted in utero is limited by immune-independent mechanisms. Blood Cells Mol Dis 31:291-7
Vogler, C; Barker, J; Sands, M S et al. (2001) Murine mucopolysaccharidosis VIL: impact of therapies on the phenotype, clinical course, and pathology in a model of a lysosomal storage disease. Pediatr Dev Pathol 4:421-33
Vogler, C; Levy, B; Galvin, N et al. (2001) A novel model of murine mucopolysaccharidosis type VII due to an intracisternal a particle element transposition into the beta-glucuronidase gene: clinical and pathologic findings. Pediatr Res 49:342-8
Soper, B W; Lessard, M D; Vogler, C A et al. (2001) Nonablative neonatal marrow transplantation attenuates functional and physical defects of beta-glucuronidase deficiency. Blood 97:1498-504
Barker, J E; Deveau, S; Lessard, M et al. (2001) In utero fetal liver cell transplantation without toxic irradiation alleviates lysosomal storage in mice with mucopolysaccharidosis type VII. Blood Cells Mol Dis 27:861-73
Barker, J E; Wandersee, N J (1999) Thrombosis in heritable hemolytic disorders. Curr Opin Hematol 6:71-5

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