There are many pathways and processes that appear to regulate the rate of aging and our susceptibility to age-related diseases such as neurodegeneration, atherosclerosis and cancer. One emerging process that has been increasingly implicated is the depletion, exhaustion or age-related dysfunction of adult stem cells. The mechanism behind why or how stem cells age has not been extensively studied. We have focused on the connection between intracellular metabolism and stem cell aging. Our hypothesis is that the control of metabolism and intracellular reactive oxygen species (ROS) within stem and progenitor cells is a key component of stem cell maintainence. Furthermore, we hypothesize that many of the genes implicated in stem cell regulation will also influnce the underlying metabolism of these cells. We have recently made an interesting connection between the Polycomb regulator Bmi1 and intracellular metabolism (Liu et al., Nature, 2009). Previous work has demonstrated that the absence of Bmi1 leads to a near total failure of stem cell self-renewal. Thus, Bmi1 activity and by extension Polycomb epigenetic regulation, is required to maintain both the hematopoietic an neural stem cell compartment. Our results also suggested that Bmi1 has important functions in regulating mitochondrial function as well as ROS homeostasis. In particular, in the absence of Bmi1, levels of ROS increase and are sufficient to activate the DNA damage response (DDR) pathways. We have also probed the connection between other regulators of stem cell biology and metabolism. One of our interests has been the connection between the Wnt signaling pathway and metabolism. Our recent data suggest that Wnt signaling plays an important role in mammalain metabolism particularly in the response of the liver to starvation (Liu et al, 2011). Our current efforts are to use additional genetic models to probe the relationship between mitochondrial function and stem cell function.This includes studies on the mTOR pathway that we believe may regulate life span by altering stem cell function (Wu et al, in preparation). we are also interested in mechanisms that regulate redox homeostasis in stem cells and somatic tissues.

Project Start
Project End
Budget Start
Budget End
Support Year
3
Fiscal Year
2012
Total Cost
$836,525
Indirect Cost
Name
National Heart, Lung, and Blood Institute
Department
Type
DUNS #
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Sun, Nuo; Youle, Richard J; Finkel, Toren (2016) The Mitochondrial Basis of Aging. Mol Cell 61:654-666
Liu, Shihui; Liu, Jie; Ma, Qian et al. (2016) Solid tumor therapy by selectively targeting stromal endothelial cells. Proc Natl Acad Sci U S A 113:E4079-87
Sukumar, Madhusudhanan; Liu, Jie; Mehta, Gautam U et al. (2016) Mitochondrial Membrane Potential Identifies Cells with Enhanced Stemness for Cellular Therapy. Cell Metab 23:63-76
Nomura, Mitsunori; Liu, Jie; Rovira, Ilsa I et al. (2016) Fatty acid oxidation in macrophage polarization. Nat Immunol 17:216-7
Ma, Xinran; Xu, Lingyan; Alberobello, Anna Teresa et al. (2015) Celastrol Protects against Obesity and Metabolic Dysfunction through Activation of a HSF1-PGC1? Transcriptional Axis. Cell Metab :
Finkel, Toren (2015) The metabolic regulation of aging. Nat Med 21:1416-23
Sun, Nuo; Finkel, Toren (2015) Cardiac mitochondria: a surprise about size. J Mol Cell Cardiol 82:213-5
Ni, Ting; Wei, Gang; Shen, Ting et al. (2015) MitoRCA-seq reveals unbalanced cytocine to thymine transition in Polg mutant mice. Sci Rep 5:12049
Liu, Julia; Finkel, Toren (2014) Aging: the blurry line between life and death. Curr Biol 24:R610-3
Holmström, Kira M; Finkel, Toren (2014) Cellular mechanisms and physiological consequences of redox-dependent signalling. Nat Rev Mol Cell Biol 15:411-21

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