Abstract

Although the influence of metabolic rate on longevity has been studied and debated for decades, the cause:effect relationship between different parameters of energy metabolism and the process of aging is poorly understood and controversial. Hypopituitary Ames dwarf (Prop1df) mice and growth hormone receptor deleted (GHRKO) mice are remarkably long-lived and exhibit many features of delayed, slower and healthy aging. Many phenotypic characteristics shared by these mutants are believed to represent mechanisms of extended longevity. These characteristics include increased oxygen consumption (VO2) per gram of total or lean body mass and reduced respiratory quotient (RQ = respiratory exchange ratio, RER), indicative of increased reliance on lipids as metabolic fuel. Intriguingly, the increase in VO2 and the reduction in RQ in Ames dwarf and GHRKO mice disappear or are severely attenuated after 24 hours of acclimation to thermoneutral temperature. From these novel findings, we suspect that increased heat loss and the consequent increase in energy demand for thermogenesis in these diminutive mutants induce alterations in energy metabolism (increased VO2 and fatty acids ? oxidation; reduced RQ) that promote delayed, healthy aging and extended longevity. We hypothesize that chronic exposure of Ames dwarf and GHRKO mice to thermoneutral temperature will accelerate aging and reduce or eliminate their longevity advantage. We further hypothesize that chronic activation of thermogenesis in genetically normal (wild type) animals by exposure to reduced environmental temperature will induce metabolic characteristics that are associated with the delayed aging and extended longevity seen in GH-related mutants and thus lead to a slower rate of aging. As the first step in testing these hypotheses, we will determine whether characteristics associated with delayed aging are normalized by extended (weeks to months) exposure of long-lived mutant animals to thermoneutral environment and whether they can be induced by extended exposure of normal animals to reduced environmental temperature.
Two Specific Aims are proposed.
Specific Aim 1. To determine whether chronic exposure of adult Ames dwarf and GHRKO mice to thermoneutral ambient temperature (30C) will rescue (normalize) energy metabolism (as assessed by measurements of V02, RQ), glucose homeostasis, circulating adiponectin, IL-6 and lipid levels and expression of genes related to mitochondrial uncoupling in brown and white adipose tissue, metabolism, inflammation, insulin and mTOR signaling.
Specific Aim 2. To determine whether chronic exposure of adult normal (wild type) mice from the same strains to reduced environmental temperature (17C) will induce alterations in thermogenesis, energy metabolism, glucose homeostasis, adipokine levels and expression of selected genes resembling those observed in long-lived GH-related mutants exposed to standard animal room temperature (23C).

Public Health Relevance

Modern trends of reduced physical activity, abundance of high energy food and increasing incidence of metabolic disorders in both wealthy and developing countries emphasize a critical need for elucidating the role of energy metabolism in health and disease. The proposed studies address these issues by identifying interactive effects of ambient temperature and mammalian longevity genes on characteristics that predict healthy aging and extended longevity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21AG051869-01
Application #
9017315
Study Section
Integrative Physiology of Obesity and Diabetes Study Section (IPOD)
Program Officer
Fridell, Yih-Woei
Project Start
2016-05-01
Project End
2018-04-30
Budget Start
2016-05-01
Budget End
2017-04-30
Support Year
1
Fiscal Year
2016
Total Cost
Indirect Cost

  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

Hascup, Erin R; Broderick, Sarah O; Russell, Mary K et al. (2018) Diet-Induced Insulin Resistance Elevates Hippocampal Glutamate as well as VGLUT1 and GFAP Expression in A?PP/PS1 Mice. J Neurochem :
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
Householder, Lara A; Comisford, Ross; Duran-Ortiz, Silvana et al. (2018) Increased fibrosis: A novel means by which GH influences white adipose tissue function. Growth Horm IGF Res 39:45-53
Darcy, Justin; McFadden, Samuel; Fang, Yimin et al. (2018) Increased environmental temperature normalizes energy metabolism outputs between normal and Ames dwarf mice. Aging (Albany NY) 10:2709-2722
Darcy, Justin; McFadden, Samuel; Bartke, Andrzej (2017) Altered structure and function of adipose tissue in long-lived mice with growth hormone-related mutations. Adipocyte 6:69-75
Troike, Katie M; Henry, Brooke E; Jensen, Elizabeth A et al. (2017) Impact of Growth Hormone on Regulation of Adipose Tissue. Compr Physiol 7:819-840
Fang, Yimin; McFadden, Samuel; Darcy, Justin et al. (2017) Differential effects of early-life nutrient restriction in long-lived GHR-KO and normal mice. Geroscience 39:347-356
Bartke, Andrzej (2017) Somatic growth, aging, and longevity. NPJ Aging Mech Dis 3:14
Ratajczak, Mariusz Z; Bartke, Andrzej; Darzynkiewicz, Zbigniew (2017) Prolonged Growth Hormone/Insulin/Insulin-like Growth Factor Nutrient Response Signaling Pathway as a Silent Killer of Stem Cells and a Culprit in Aging. Stem Cell Rev 13:443-453
Darcy, Justin; Bartke, Andrzej (2017) Functionally enhanced brown adipose tissue in Ames dwarf mice. Adipocyte 6:62-67

Showing the most recent 10 out of 13 publications