Abstract

TITLE OF PROJECT eNAMPT-mediated adipo-hypothalamic communication for NAD+ production and aging ABSTRACT In recent years, nicotinamide adenine dinucleotide (NAD+) metabolism has emerged as a central topic in the field of aging and longevity research. It has been established that NAD+ availability declines over age at a systemic level, triggering a variety of age-associated pathophysiological changes in diverse model organisms. In mammalian NAD+ biosynthesis, nicotinamide phosphoribosyltransferase (NAMPT) is the key enzyme that converts nicotinamide and 5?-phosphoribosyl-pyrophosphate to nicotinamide mononucleotide (NMN), an important NAD+ intermediate. Interestingly, there are two distinct forms of NAMPT in mammals: intra- and extracellular NAMPT (iNAMPT and eNAMPT, respectively). We have previously demonstrated that eNAMPT mediates a novel intertissue communication system between adipose tissue and the hypothalamus, regulating hypothalamic NAD+ levels and functions. We have now found that eNAMPT is carried in exosomes through the circulation in mice and humans. Exosomal eNAMPT is internalized into primary hypothalamic neurons and enhances NAD+ biosynthesis intracellularly. The genetically engineered mice that can maintain higher levels of exosomal eNAMPT at old ages exhibit a variety of anti-aging phenotypes and a significant extension of healthspan. These new findings demonstrate a novel systemic mechanism that regulates the process of aging and determines healthspan/lifespan, driven by an exosome-mediated delivery of eNAMPT. Thus, we hypothesize that exosomal eNAMPT is delivered to specific tissues through the interaction with a specific receptor-like protein and regulates various tissue functions, including the hippocampus-dependent cognitive functions. The K53R mutant of NAMPT, whose secretion is enhanced, could be used as a genetically engineered biologic that mitigates age-associated functional decline in mice. We will address this hypothesis by the following specific aims: 1) To elucidate the mechanism of exosomal eNAMPT targeting, we will examine the requirement of the NAMPT protein structure and also test a potential receptor candidate for exosomal eNAMPT to be internalized, 2) to further analyze the effects of supplementing eNAMPT-containing exosomes in aged mice, we will analyze their effect on the hippocampus-mediated cognitive functions, and 3) to test eNAMPT as an anti-aging biologic, we will examine the effects of eNAMPT mutants encapsulated into exosomes on cognitive, behavioral, and other tissue functions in aged mice. Thus, the anticipated outcome of the proposed research will open a new avenue to understand how systemic NAD+ homeostasis regulates aging and longevity and develop a novel anti-aging intervention by using exosomal eNAMPT as a biologic.

Public Health Relevance

Our long-term goal is to understand a systemic regulatory network for aging/longevity control in mammals, and to translate that knowledge into an effective intervention to prevent and treat age-associated pathophysiology in humans. We have recently found that adipose tissue plays a critical role in regulating other tissue functions through the secretion of a key enzyme that contributes to the biosynthesis of NAD+, an essential currency of cellular energy metabolism. In this new research proposal, we will investigate the physiological importance of this systemic NAD+-regulatory mechanism that controls mammalian aging and longevity. The anticipated results will further advance our understanding of mammalian aging and longevity control and contribute to the development of a possible intervention to achieve better healthspan in our aging society.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
2R01AG047902-06
Application #
9739129
Study Section
Cellular Mechanisms in Aging and Development Study Section (CMAD)
Program Officer
Mackiewicz, Miroslaw
Project Start
2014-08-15
Project End
2024-04-30
Budget Start
2019-05-01
Budget End
2020-04-30
Support Year
6
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Snyder-Warwick, Alison K; Satoh, Akiko; Santosa, Katherine B et al. (2018) Hypothalamic Sirt1 protects terminal Schwann cells and neuromuscular junctions from age-related morphological changes. Aging Cell :e12776
Yoshino, Jun; Baur, Joseph A; Imai, Shin-Ichiro (2018) NAD+ Intermediates: The Biology and Therapeutic Potential of NMN and NR. Cell Metab 27:513-528
Johnson, Sean; Wozniak, David F; Imai, S (2018) CA1 Nampt knockdown recapitulates hippocampal cognitive phenotypes in old mice which nicotinamide mononucleotide improves. NPJ Aging Mech Dis 4:10
Satoh, Akiko; Imai, Shin-Ichiro; Guarente, Leonard (2017) The brain, sirtuins, and ageing. Nat Rev Neurosci 18:362-374
Lin, Jonathan B; Kubota, Shunsuke; Ban, Norimitsu et al. (2016) NAMPT-Mediated NAD(+) Biosynthesis Is Essential for Vision In Mice. Cell Rep 17:69-85
Stromsdorfer, Kelly L; Yamaguchi, Shintaro; Yoon, Myeong Jin et al. (2016) NAMPT-Mediated NAD(+) Biosynthesis in Adipocytes Regulates Adipose Tissue Function and Multi-organ Insulin Sensitivity in Mice. Cell Rep 16:1851-60
Imai, Shin-Ichiro (2016) The NAD World 2.0: the importance of the inter-tissue communication mediated by NAMPT/NAD+/SIRT1 in mammalian aging and longevity control. NPJ Syst Biol Appl 2:16018
Yoon, Myeong Jin; Yoshida, Mitsukuni; Johnson, Sean et al. (2015) SIRT1-Mediated eNAMPT Secretion from Adipose Tissue Regulates Hypothalamic NAD+ and Function in Mice. Cell Metab 21:706-17
Stein, Liana Roberts; Zorumski, Charles F; Imai, Shin-Ichiro et al. (2015) Nampt is required for long-term depression and the function of GluN2B subunit-containing NMDA receptors. Brain Res Bull 119:41-51