Abstract

Prenatal developmental events can influence adult phenotype and the risk of adult disease. However, it is unknown whether (or to what extent) the actions of hormones and nutrients on early postnatal growth can influence mammalian aging, adult health and longevity. We have recently shown that: (i) the remarkable extension of longevity in hypopituitary Ames dwarf mice can be completely reversed by a six-week course of growth hormone (GH) injections started at the age of 2 weeks;and (ii) limiting nutrient availability during the first three weeks of postnatal life by increasing the numbers of pups in a litter increases both median and maximal lifespan in genetically normal mice. Based on these novel and largely unexpected findings, we hypothesize that the period of rapid postnatal growth represents a critical time window for development of lifelong metabolic and other phenotypic characteristics that influence-and likely predict-longevity and functionality during old age. To test the validity of this hypothesis, we will examine the impact of modestly reducing the amount of available nutrients during suckling (or suckling and the immediate post-weaning period) in normal mice, and the effects of early (starting at one or two weeks) as compared to late (starting at eight weeks) GH replacement therapy in Ames dwarfs and in GHRH-/- mice with isolated GH deficiency. Endpoints will include both longevity and a series of age-sensitive traits related to health span, including indices of immune function, locomotion, stress resistance, and cataract development. We will pay special attention to endpoints related to fuel metabolism, with tests of somatotropic and insulin signaling, pancreatic beta cell function, metabolic rate and respiratory quotient, and expression of GH and insulin-related genes in the liver, skeletal muscle, and both subcutaneous and intra-abdominal (visceral) fat. Lastly, we will in parallel studies see whether early life nutrient limitation, before or before and after weaning, will benefit GHRKO (Laron dwarf) mice, which unlike Ames dwarf mice fail to benefit from calorie restriction (CR) when CR is started at the age of 2 months. Results of the proposed studies will be used to accept or reject specific hypotheses concerning mechanisms by which early hormonal or nutritional interventions can influence aging and longevity. In sum, we will take our studies of the interactions of longevity genes and CR in a novel direction to address the impact of transient changes in nutritional and hormonal signals during early postnatal life on mammalian aging, health span and longevity. Results of these studies will address critical gaps in the present understanding of developmental influences on aging and set a stage for addressing the relationships between early nutrition, growth and adult health which are of major public health significance.

Public Health Relevance

Using normal and mutant mice, we have recently obtained novel and largely unexpected evidence that a modest reduction of nutrient availability during early postnatal development can produce significant extension of longevity, and that absence of growth hormone signaling during this brief period may be sufficient to produce a dramatic increase in life expectancy. In the proposed work we will identify mechanisms of these novel effects and determine whether the observed life extension is associated with positive impacts on health span. These studies address several issues of major public health significance including detrimental effects of early over nutrition and an exciting possibility that aging might be postponed and lifespan extended by judicious life style and diet modifications in children and adolescents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
3R01AG019899-13S1
Application #
8837733
Study Section
Special Emphasis Panel (ZRG1-CB-R (02))
Program Officer
Finkelstein, David B
Project Start
2001-09-30
Project End
2017-04-30
Budget Start
2014-06-01
Budget End
2015-04-30
Support Year
13
Fiscal Year
2014
Total Cost
$36,273
Indirect Cost
$11,681

  Institution

Name
Southern Illinois University School of Medicine
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
038415006
City
Springfield
State
IL
Country
United States
Zip Code
62794

  Publications

Fang, Yimin; Hill, Cristal M; Darcy, Justin et al. (2018) Effects of rapamycin on growth hormone receptor knockout mice. Proc Natl Acad Sci U S A 115:E1495-E1503
Wang, Xin; Darcy, Justin; Cai, Chuan et al. (2018) Intestinal immunity in hypopituitary dwarf mice: effects of age. Aging (Albany NY) 10:358-370
Piazza, VerĂ³nica G; Bartke, Andrzej; Miquet, Johanna G et al. (2017) Analysis of Different Approaches for the Selection of Reference Genes in RT-qPCR Experiments: A Case Study in Skeletal Muscle of Growing Mice. Int J Mol Sci 18:
Bartke, Andrzej (2017) Somatic growth, aging, and longevity. NPJ Aging Mech Dis 3:14
Hine, Christopher; Kim, Hyo-Jeong; Zhu, Yan et al. (2017) Hypothalamic-Pituitary Axis Regulates Hydrogen Sulfide Production. Cell Metab 25:1320-1333.e5
Bartke, Andrzej; Darcy, Justin (2017) GH and ageing: Pitfalls and new insights. Best Pract Res Clin Endocrinol Metab 31:113-125
Cole, John J; Robertson, Neil A; Rather, Mohammed Iqbal et al. (2017) Diverse interventions that extend mouse lifespan suppress shared age-associated epigenetic changes at critical gene regulatory regions. Genome Biol 18:58
Petkovich, Daniel A; Podolskiy, Dmitriy I; Lobanov, Alexei V et al. (2017) Using DNA Methylation Profiling to Evaluate Biological Age and Longevity Interventions. Cell Metab 25:954-960.e6
Saccon, Tatiana D; Moreira, Fabiana; Cruz, Luis A et al. (2017) Ovarian aging and the activation of the primordial follicle reserve in the long-lived Ames dwarf and the short-lived bGH transgenic mice. Mol Cell Endocrinol 455:23-32
Darcy, Justin; Bartke, Andrzej (2017) Functionally enhanced brown adipose tissue in Ames dwarf mice. Adipocyte 6:62-67

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