Abstract

In 1959, spontaneous autoantibody production was discovered in New Zealand mice. Subsequent studies demonstrated a striking similarity of New Zealand black mice to patients with idiopathic-acquired hemolytic anemia and New Zealand black x white F?1? hybrids to humans with systemic lupus erythematosus. Numerous experiments have indicated that genetic and/or viral interrelationships with lymphoid elements are critical for disease pathogenesis in mice. However, the precise role of the thymus and spleen and their respective subpopulations in the development of autoimmunity and lymphoproliferative disease remains unclear. It is intended to create unique animal models to resolve these issues. These models are production of congenitally athymic (nude) New Zealand black (NZB), New Zealand white (NZW) and NZBxNZW F?1? mice, and New Zealand mice congenic for the Xid gene of CBA/N. The natural history and immune responsiveness of these mutant colonies will be studied and compared with littermate controls. The mechanism of polyclonal expansion of B cells and subsequent antibody production in New Zealand mice remains a critical question. We have been studying the requirements for autoantibody production both in NZB mice as well as NZB mice cogenic with the Xid gene of CBA/N mice. We have attempted to alter the immunologic phenotype of NZB.Xid mice by transfer of cells from young and old NZB mice. There was little difficulty in restoring normal levels of serum IgM, IgG3, splenic Lyb-5 cells and response to DNP-Ficoll in young NZB.Xid mice that were injected with young NZB bone marrow cells. Although such animals had an almost immediate change in their immune profile to values characteristic of NZB mice, they required, much like unmanipulated NZB mice, a latency period of an additional 6 months before autoantibodies were detected. In contrast, adult NZB.Xid mice, who likewise developed an immune profile similar to NZB after transfer of bone marrow cells from young NZB mice, began to express autoantibodies immediately without any latency period. NZB.Xid mice who were recipients of adult NZB bone marrow cells did not show sustained autoantibody production, reflecting the limited state of B-cell precursors in adult NZB mice. Thus, the age of both donor cells and the age of recipient mice are critical factors for determining the latency period and the age at which autoantibodies will appear. Similarly, we attempted to alter the production of autoantibodies in NZB mice that were irradiated and injected with bone marrow cells from NZB.Xid animals. NZB mice had a major amelioration of disease when they received cell transfers from young NZB.Xid mice. This amelioration, which included the acquisition of the immune profile of NZB.Xid animals, was not seen in adult NZB mice that were recipients of young NZB cells. We suggest that, although Lyb-5 cells may be the effective mechanism for autoantibody production, there are other interacting influences that may selectively turn on or turn off autoantibodies and that are required and are responsible for the latency period. Further, specific experiments in transplantation and cell transfer of thymus and spleen from syngeneic mice of different serial ages will be designed to identify the relationships between alterations in lymphoid subpopulations with age and development of autoimmunity and lymphoproliferative disease. (SR)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA020816-12
Application #
3165394
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1976-06-30
Project End
1990-06-30
Budget Start
1987-07-01
Budget End
1988-06-30
Support Year
12
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
University of California Davis
Department
Type
Schools of Medicine
DUNS #
094878337
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Lian, Zhe-Xiong; Kita, Hiroto; Okada, Tomoyuki et al. (2002) Increased frequency of pre-pro B cells in the bone marrow of New Zealand Black (NZB) mice: implications for a developmental block in B cell differentiation. Dev Immunol 9:35-45
Lian, Zhe-Xiong; Okada, Tomoyuki; Kita, Hiroto et al. (2002) Age-related alterations in the lymphohematopoietic and B-lineage precursor populations in NZB mice. Stem Cells 20:293-300
Takeoka, Y; Whitmer, K J; Chen, S Y et al. (1995) Thymic epithelial cell abnormalities in (NZB x H-2u)F1 mice. Clin Immunol Immunopathol 76:297-307
Yoshida, S H; Bruenner, B A; German, J B et al. (1995) Decrease of 12-hydroxyeicosatetraenoic acid production in mouse lungs following dietary oleic anilide consumption: implications for the toxic oil syndrome. Arch Environ Contam Toxicol 28:524-8
Merino, R; Iwamoto, M; Gershwin, M E et al. (1994) The Yaa gene abrogates the major histocompatibility complex association of murine lupus in (NZB x BXSB)F1 hybrid mice. J Clin Invest 94:521-5
Lai, L T; Naiki, M; Yoshida, S H et al. (1994) Dietary Platycladus orientalis seed oil suppresses anti-erythrocyte autoantibodies and prolongs survival of NZB mice. Clin Immunol Immunopathol 71:293-302
Naiki, M; Yoshida, S H; Ansari, A A et al. (1994) Activation of autoreactive T-cell clones from NZB.H-2bm12 mice. J Autoimmun 7:275-90
Watanabe, Y; Yoshida, S H; Ansari, A A et al. (1994) The contribution of H-2bm12 and non H-2 background genes on murine lupus in NZB.H-2bm12/b mice. J Autoimmun 7:153-64
Watanabe, Y; Naiki, M; Wilson, T et al. (1993) Thymic microenvironmental abnormalities and thymic selection in NZB.H-2bm12 mice. J Immunol 150:4702-12
Berger, A; German, J B; Chiang, B L et al. (1993) Influence of feeding unsaturated fats on growth and immune status of mice. J Nutr 123:225-33

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