Abstract

Sarcopenia is the loss of muscle mass and muscle strength that occurs in aging people. The resulting loss of muscle strength contributes to impairments in physical functioning in older people and serves as a risk factor for loss of independence, need for nursing home placement, and ultimately mortality. Currently there are no treatments for sarcopenia and the cause(s) are incompletely understood. Hence there is a need to identify new ways to study sarcopenia and identify mechanisms that may be amenable to intervention. During aging, C. elegans develops sarcopenia, and mutations in the insulin/IGF-1 receptor daf-2 delay the development of sarcopenia. We have found that mvk-1, which is the worm homolog of the mevalonate kinase gene, is required for this delay. Mevalonate kinase is involved in the conversion of mevalonate to isoprenoids, ubiquinone, and cholesterol, and this enzyme lies in a metabolic pathway targeted by the commonly used statin medications. Statins have well-known toxic effects on muscle, but the cause of these adverse effects is still under active study. Among ubiquinone, isoprenoids, and cholesterol, we have found ubiquinone to be the required output of the mevalonate pathway with regards to muscle aging. Ubiquinone is the electron acceptor for complex I and complex II of the mitochondrial electron transport chain. Prior work has shown that daf-2 mutants have elevated complex I and II activity, and mitochondrial activity is better preserved in the daf-2 mutants during aging compared to wild-type animals. Additionally, complex I activity in muscle and other tissues declines during aging in vertebrates. These findings led us to hypothesize that mitochondrial activity is a driver of the development of sarcopenia during aging and perhaps is involved in statin toxicity. To test this hypothesis we propose to (1) examine muscle structure during aging in wild-type worms, daf-2 mutants, and daf-2 mutants with reduced ubiquinone levels;(2) test whether aging and low ubiquinone levels impair mitochondrial ATP production or (3) lead to increased ROS production during aging;(4) determine the consequences of directly manipulating complex I activity both up and down on muscle function;and (5) conduct a pilot compound screen using drugs used for genetic mitochondrial illnesses to test for improvements in muscle function during aging. A novel aspect of our work will be the use of recently developed fluorescent proteins to longitudinally and non-invasively measure cellular ATP levels and ROS production in the muscles of aging animals. Together our project can provide insights into the roles of mitochondrial dysfunction in muscle during aging or in response to impaired ubiquinone synthesis due to medications such as statins.

Public Health Relevance

Our project studies how aging and ubiquinone production influence muscle structure and function as well as mitochondrial function. We believe that both aging and the use of statin medications can impair mitochondrial function and lead to similar types of adverse changes in muscle. From this research, we hope to gain insights that can lead to new treatments to preserve or improve muscle function in older people and to perhaps make the use of statin medications safer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG044768-03
Application #
8708727
Study Section
Skeletal Muscle Biology and Exercise Physiology Study Section (SMEP)
Program Officer
Williams, John
Project Start
2013-07-01
Project End
2017-04-30
Budget Start
2014-07-01
Budget End
2015-04-30
Support Year
3
Fiscal Year
2014
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Kang, Donghoon; Kirienko, Daniel R; Webster, Phillip et al. (2018) Pyoverdine, a siderophore from Pseudomonas aeruginosa, translocates into C. elegans, removes iron, and activates a distinct host response. Virulence 9:804-817
Qi, Wenbo; Gutierrez, Gloria E; Gao, Xiaoli et al. (2017) The ?-3 fatty acid ?-linolenic acid extends Caenorhabditis elegans lifespan via NHR-49/PPAR? and oxidation to oxylipins. Aging Cell 16:1125-1135
Cai, Liquan; Fisher, Alfred L; Huang, Haochu et al. (2016) CRISPR-mediated genome editing and human diseases. Genes Dis 3:244-251
Munkácsy, Erin; Khan, Maruf H; Lane, Rebecca K et al. (2016) DLK-1, SEK-3 and PMK-3 Are Required for the Life Extension Induced by Mitochondrial Bioenergetic Disruption in C. elegans. PLoS Genet 12:e1006133
Ipson, Brett R; Fisher, Alfred L (2016) Roles of the tyrosine isomers meta-tyrosine and ortho-tyrosine in oxidative stress. Ageing Res Rev 27:93-107
Keith, Scott A; Maddux, Sarah K; Zhong, Yayu et al. (2016) Graded Proteasome Dysfunction in Caenorhabditis elegans Activates an Adaptive Response Involving the Conserved SKN-1 and ELT-2 Transcription Factors and the Autophagy-Lysosome Pathway. PLoS Genet 12:e1005823
Guo, Wenhuan; Keener, Anne L; Jing, Yifeng et al. (2015) FOXA1 modulates EAF2 regulation of AR transcriptional activity, cell proliferation, and migration in prostate cancer cells. Prostate 75:976-87
Ferguson, Annabel A; Bilonick, Richard A; Buchanich, Jeanine M et al. (2015) How Well Do Raters Agree on the Development Stage of Caenorhabditis elegans? PLoS One 10:e0132365
Wang, Hongning; Karadge, Uma; Humphries 4th, William H et al. (2014) Analyzing cell physiology in C. elegans with fluorescent ratiometric reporters. Methods 68:508-17
Cai, Liquan; Wang, Dan; Fisher, Alfred L et al. (2014) Identification of a genetic interaction between the tumor suppressor EAF2 and the retinoblastoma protein (Rb) signaling pathway in C. elegans and prostate cancer cells. Biochem Biophys Res Commun 447:292-8

Showing the most recent 10 out of 12 publications