Abstract

PROJECT 1: MITOCHONDRIAL ROS AND CARDIAC AGING ? PROJECT SUMMARY/ABSTRACT Aging is accompanied by slowly progressive and irreversible structural changes and functional declines in the heart that include increased prevalence of left ventricular hypertrophy, decline in diastolic function, and a decline in exercise capacity that contributes to frailty in the elderly. Extending work begun with mitochondrial targeted catalase, mCAT, we have recently demonstrated that short term (8 week) treatment with the mitochondrial protective drug SS-31 ?rejuvenates? cardiac function in old mice, reducing hypertrophy, improving diastolic function and remodeling the cardiac structure and proteome to a more youthful state. We hypothesize that SS-31 enhanced mitochondrial energetics and redox signaling subsequently result in remodeling of the cardiomyocyte and extracellular matrix to a more youthful state. This proposal will define the mechanisms that mediate both acute mitochondrial (Aim 1) and subacute cardiomyocyte and extracellular matrix (Aim 2) rejuvenating effects. As this approach offers the promise of substantial improvement in cardiac health of older humans, Aim 3 will help establish the potential longer-term benefits of these changes to murine healthspan and lifespan. Specifically, in Aim 1 In order to test the hypothesis that treatment with SS-31 restores redox and energy dependent signaling that results in improved mitochondrial structure and function we will measure mitochondrial and cardiac function, comparing and contrasting the mechanisms of mCAT, SS- 20 and SS-31 effects and their ability reverse cardiac aging in old mice and to protect mice challenged with doxorubicin to disrupt electron transport chain function.
In Aim 2 we will determine the mechanisms by which SS-31 treatment of old mice rejuvenates cardiomyocytes and extracellular matrix (ECM) to improve aging diastolic function and cardiac performance.
Aim 3 is shared across the entire P01, and will establish the translational benefits of SS-31 by determining whether SS31 can attenuate the decline of murine healthspan and extend lifespan after SS-31 is continuously delivered to mice beginning at middle age on regular and high fat diets. In this aim Project 1 will focus on cardiac healthspan.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG001751-36
Application #
9918232
Study Section
Special Emphasis Panel (ZAG1)
Project Start
Project End
Budget Start
2020-04-01
Budget End
2021-03-31
Support Year
36
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Type
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Basisty, Nathan B; Liu, Yuxin; Reynolds, Jason et al. (2018) Stable Isotope Labeling Reveals Novel Insights Into Ubiquitin-Mediated Protein Aggregation With Age, Calorie Restriction, and Rapamycin Treatment. J Gerontol A Biol Sci Med Sci 73:561-570
Kramer, Philip A; Duan, Jicheng; Gaffrey, Matthew J et al. (2018) Fatiguing contractions increase protein S-glutathionylation occupancy in mouse skeletal muscle. Redox Biol 17:367-376
Zhang, Huiliang; Gong, Guohua; Wang, Pei et al. (2018) Heart specific knockout of Ndufs4 ameliorates ischemia reperfusion injury. J Mol Cell Cardiol 123:38-45
Ge, Xuan; Ciol, Marcia A; Pettan-Brewer, Christina et al. (2017) Self-motivated and stress-response performance assays in mice are age-dependent. Exp Gerontol 91:1-4
Sweetwyne, Mariya T; Pippin, Jeffrey W; Eng, Diana G et al. (2017) The mitochondrial-targeted peptide, SS-31, improves glomerular architecture in mice of advanced age. Kidney Int 91:1126-1145
Liu, Sophia Z; Marcinek, David J (2017) Skeletal muscle bioenergetics in aging and heart failure. Heart Fail Rev 22:167-178
Basisty, Nathan; Dai, Dao-Fu; Gagnidze, Arni et al. (2016) Mitochondrial-targeted catalase is good for the old mouse proteome, but not for the young: 'reverse' antagonistic pleiotropy? Aging Cell 15:634-45
Treuting, P M; Snyder, J M; Ikeno, Y et al. (2016) The Vital Role of Pathology in Improving Reproducibility and Translational Relevance of Aging Studies in Rodents. Vet Pathol 53:244-9
Ahn, Eun Hyun; Lee, Seung Hyuk; Kim, Joon Yup et al. (2016) Decreased Mitochondrial Mutagenesis during Transformation of Human Breast Stem Cells into Tumorigenic Cells. Cancer Res 76:4569-78
Kruse, Shane E; Karunadharma, Pabalu P; Basisty, Nathan et al. (2016) Age modifies respiratory complex I and protein homeostasis in a muscle type-specific manner. Aging Cell 15:89-99

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