Abstract

This project has two principal goals: (1) to identify regions of the mouse genome that encode genes that contribute significantly to longevity; and (2) to use selective breeding strategies to produce strains of mice that age at different rates. The experiments will utilize genetically heterogeneous mice bred by a four-way Cross between (C57BL/6 x SJL)F1 females and (AKR x DBA/2)F1 males (""""""""HET"""""""" mice). The analytical genetic study will begin by typing 200 HET mice at each of 190 informative loci, using PCR-based amplification of primer pairs that discriminate among 2 or more of the grandparental inbred strains. A second cohort of 200 HET mice will then be genotyped using the original battery of primer pairs plus a second set of 95 probes selected to provide higher resolution in regions suggested to be of particular interest during the initial screen. Mice in the second cohort will also be tested at 6 and 18 months of age for indices of age-related immune decline: the proportion of memory T cells within the CD4 helper and CD8 killer T cell subsets. Each of the HET mice will be sacrificed when moribund to obtain longevity and pathology data. An interval-based mapping strategy will then identify quantitative trait loci (QTL) that influence longevity. Parallel analyses will establish whether these, or other QTL, also influence the incident rates of major disease processes, or influence the rate of physiological aging as measured by shifts in T lymphocyte subset composition. The selective breeding study will generate lines of mice, starting from HET stock, based on differences in (a) early life hemagglutinin response; or (b) distribution of reproductive effort. These selective criteria have been chosen because each can be assayed within the first 8 months of life, and because theoretical and experimental considerations suggest that each trait may be influenced by genes that pleiotropically affect aging rate and hence longevity. The selection protocols incorporate independent replication (bidirectional for the hemagglutinin protocol) and parallel development of unselected control stocks for genetic and phenotypic comparison to the selected lines. When breeding has produced lines of mice that differ in the selected criteria, groups of animals from each selected line will be set aside for determination of longevity, pathologic study, and genotyping using primer sets developed by analysis of the HBT stock. RNA from old and young HET mice, and later from selectively bred animals, will be provided to Dr. Judith Campisi for a collaborative study of age- related alterations in gene expression in monotypic cell preparations. Long-term goals include (a) selection of mice based on genotype at QTL identified through analysis of HET mice; (b)positional cloning of genes within regions identified by QTL analysis of HET and selected mice; and (c) detailed physiological analysis of proposed anti-aging defenses in mice of short- and long-lived genotypes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
3R01AG011687-05S1
Application #
2863745
Study Section
Biological and Clinical Aging Review Committee (BCA)
Program Officer
Mccormick, Anna M
Project Start
1993-09-01
Project End
1999-03-31
Budget Start
1998-09-15
Budget End
1999-03-31
Support Year
5
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Pathology
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Miller, Richard A; Kreider, Jaclynn; Galecki, Andrzej et al. (2011) Preservation of femoral bone thickness in middle age predicts survival in genetically heterogeneous mice. Aging Cell 10:383-91
Swindell, William R; Harper, James M; Miller, Richard A (2008) How long will my mouse live? Machine learning approaches for prediction of mouse life span. J Gerontol A Biol Sci Med Sci 63:895-906
Reeves, Grant M; McCreadie, Barbara R; Chen, Shu et al. (2007) Quantitative trait loci modulate vertebral morphology and mechanical properties in a population of 18-month-old genetically heterogeneous mice. Bone 40:433-43
Harper, James M; Salmon, Adam B; Chang, Yayi et al. (2006) Stress resistance and aging: influence of genes and nutrition. Mech Ageing Dev 127:687-94
Harper, James M; Durkee, Stephen J; Smith-Wheelock, Michael et al. (2005) Hyperglycemia, impaired glucose tolerance and elevated glycated hemoglobin levels in a long-lived mouse stock. Exp Gerontol 40:303-14
Miller, Richard A; Berger, Scott B; Burke, David T et al. (2005) T cells in aging mice: genetic, developmental, and biochemical analyses. Immunol Rev 205:94-103
Testa, Julie A; Ivnik, Robert J; Boeve, Bradley et al. (2004) Confrontation naming does not add incremental diagnostic utility in MCI and Alzheimer's disease. J Int Neuropsychol Soc 10:504-12
Harper, James M; Galecki, Andrzej T; Burke, David T et al. (2004) Body weight, hormones and T cell subsets as predictors of life span in genetically heterogeneous mice. Mech Ageing Dev 125:381-90
Lipman, Ruth; Galecki, Andrzej; Burke, David T et al. (2004) Genetic loci that influence cause of death in a heterogeneous mouse stock. J Gerontol A Biol Sci Med Sci 59:977-83
Wolf, Norman; Galecki, Andrzej; Lipman, Ruth et al. (2004) Quantitative trait locus mapping for age-related cataract severity and synechia prevalence using four-way cross mice. Invest Ophthalmol Vis Sci 45:1922-9

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