Abstract

An understanding of blood cell formation, both normal and neoplastic, is dependent on firm knowledge of the dynamics of the stem cell population, from which all circulating cells are ultimately derived. We propose studies of stem cells based on our previous identification of novel phenotypes involving stem cell proliferation and differentiation. We have found that proliferative activity in the stem cell compartment varies among inbred strains of mice and preliminary evidence is consistent with the hypothesis that genetic control resides in a single locus that we know is not Fv-2. In chimeric (allophenic) mice constructed using inbred strains with different stem cell proliferative activities, erythropoiesis is skewed toward the strain characterized by greater stem cell proliferation. We plan to study the interrelationship between these two newly described phenotypes. 1. Using recombinant inbred (RI) mouse strains we plan to determine how many genes are involved in the regulation of strain-dependent stem cell proliferation. By comparing our results with a compiled RI strain distribution pattern for other phenotypes, we will determine if it is linked to any other genes and, if so, which, and where they map. 2. We will use two probes to dissect the stem cell population to determine where the proliferative difference is manifested in the hierarchy of developmentally restricted subpopulations. The first is 5-fluorouracil which selectively spares the most primitive subset and the second is a monoclonal antibody to an alloantigen expressed preferentially on the most primitive stem cells. 3. If stem cell proliferative activity is directly related to accentuated erythropoiesis in allophenic mice it follows that, in chimeras, stem cell populations should behave kinetically as they do in the syngeneic state. We will determine if genotype-specific differences in stem cell proliferation are maintained in the chimeric environment and hence if stem cell populations are autonomously regulated. 4. Our preliminary results show significant differences in hemoglobin synthesis between bone marrow cultures from inbred mouse strains. This work provides an experimental approach that we will use to understand different rates of erythropoiesis in allophenic mice. (M)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA040575-03
Application #
3180733
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1985-07-01
Project End
1988-06-30
Budget Start
1987-07-01
Budget End
1988-06-30
Support Year
3
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Texas Tech University
Department
Type
Schools of Medicine
DUNS #
609980727
City
Lubbock
State
TX
Country
United States
Zip Code
79430

  Publications

Phillips, R L; Couzens, M S; Van Zant, G (1995) Genetic factors influencing murine hematopoietic productivity in culture. J Cell Physiol 164:99-107
Yu, H; Bauer, B; Lipke, G K et al. (1993) Apoptosis and hematopoiesis in murine fetal liver. Blood 81:373-84
Phillips, R L; Reinhart, A J; Van Zant, G (1992) Genetic control of murine hematopoietic stem cell pool sizes and cycling kinetics. Proc Natl Acad Sci U S A 89:11607-11
Van Zant, G; Scott-Micus, K; Thompson, B P et al. (1992) Stem cell quiescence/activation is reversible by serial transplantation and is independent of stromal cell genotype in mouse aggregation chimeras. Exp Hematol 20:470-5
Van Zant, G; Thompson, B P; Chen, J J (1991) Differentiation of chimeric bone marrow in vivo reveals genotype-restricted contributions to hematopoiesis. Exp Hematol 19:941-9
Van Zant, G; Chen, J J; Scott-Micus, K (1991) Developmental potential of hematopoietic stem cells determined using retrovirally marked allophenic marrow. Blood 77:756-63
Van Zant, G; Holland, B P; Eldridge, P W et al. (1990) Genotype-restricted growth and aging patterns in hematopoietic stem cell populations of allophenic mice. J Exp Med 171:1547-65
Buller, R S; Van Zant, G; Eldridge, P W et al. (1989) A population of murine hematopoietic progenitors expresses an endogenous retroviral gp70 linked to the Rmcf gene and associated with resistance to erythroleukemia. J Exp Med 169:865-80
Van Zant, G; Shultz, L (1989) Hematologic abnormalities of the immunodeficient mouse mutant, viable motheaten (mev). Exp Hematol 17:81-7
Worthington, R E; Bossie-Codreanu, J; Van Zant, G (1987) Quantitation of erythroid differentiation in vitro using a sensitive colorimetric assay for hemoglobin. Exp Hematol 15:85-92