Abstract

As described in detail in our progress report, the data generated over the past three years of funding demonstrate there is a network of heterochronic gene products, including let-7 microRNAs, IMP1, Hmga2, P16lnk4a and possibly p19Arf, that regulates temporal changes in stem cell function throughout life, including stem cell aging. During the next five-year funding period we propose to expand our understanding of this network by exploring new mechanisms that regulate the increase in P16lnk4a/p19Arf expression during aging. P16lnk4a is a cyclin-dependent kinase inhibitor and the Alternative Reading Frame (Arf) at the same locus encodes the p19Arf tumor suppressor. P16lnk4a/p19Arf expression is known to increase with age in mice and humans and is considered a biomarker of aging. The increase in P16lnk4a expression contributes to the decline in stem/progenitor cell function in multiple aging tissues and we are currently testing whether the increase in p19Arf expression also decreases neural stem/progenitor cell function and the regenerative capacity of aging tissues. Mechanisms that regulate P16lnk4a/p19Arf expression during aging are of interest to expand our understanding of the heterochronic gene network and its role in stem cell aging. We have shown previously that the polycomb complex 1 component, Bmi-1, is required in the early postnatal period to maintain forebrain stem cell function by negatively regulating P16lnk4a/p19Arf expression. Similar mechanisms promote stem cell maintenance in other tissues. However, a major limitation has been the inability to test whether Bmi-1 regulates adult stem cell function or aging. All of the studies published so far on Bmi-1 function in stem cells have been performed with germline knockout mice that die by two months of age. To test whether Bmi-1 regulates adult stem cell function, stem cell aging, and the increase in P16lnk4a/p19Arf expression during aging we have generated mice bearing a floxed allele of Bmi-i. In unpublished preliminary studies we find that conditional deletion of Bmi-1 from adult neural stem/progenitor cells leads to premature declines in forebrain stem/progenitor cell function and neurogenesis as well as a profound age-related increase in P16lnk4a/p19Arf expression. The magnitude of the increase in P16lnk4a/p19Arf expression climbed sharply with age, suggesting that Bmi-1 delays stem cell aging by opposing the increase in P16lnk4a/p19Arf expression. Our data also revealed requirements for Bmi-1 to prevent age-related behavioral deficits in motor function and balance that are associated with defects in proprioception and the premature development of cataracts. We propose to test whether Bmi-1 is required to prevent premature stem cell aging and the development of neurological deficits by opposing the age-related increase in P16lnk4a/p19Arf expression.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37AG024945-13
Application #
9107773
Study Section
Special Emphasis Panel (NSS)
Program Officer
Wise, Bradley C
Project Start
2014-08-01
Project End
2019-05-31
Budget Start
2016-06-15
Budget End
2017-05-31
Support Year
13
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Texas Sw Medical Center Dallas
Department
Pediatrics
Type
Schools of Medicine
DUNS #
800771545
City
Dallas
State
TX
Country
United States
Zip Code
75390

  Publications

Agathocleous, Michalis; Meacham, Corbin E; Burgess, Rebecca J et al. (2017) Ascorbate regulates haematopoietic stem cell function and leukaemogenesis. Nature 549:476-481
Liao, Chung-Ping; Booker, Reid C; Morrison, Sean J et al. (2017) Identification of hair shaft progenitors that create a niche for hair pigmentation. Genes Dev 31:744-756
Zhou, Bo O; Yu, Hua; Yue, Rui et al. (2017) Bone marrow adipocytes promote the regeneration of stem cells and haematopoiesis by secreting SCF. Nat Cell Biol 19:891-903
Shimada, Issei S; Acar, Melih; Burgess, Rebecca J et al. (2017) Prdm16 is required for the maintenance of neural stem cells in the postnatal forebrain and their differentiation into ependymal cells. Genes Dev 31:1134-1146
Lin, Haotian; Ouyang, Hong; Zhu, Jie et al. (2016) Lens regeneration using endogenous stem cells with gain of visual function. Nature 531:323-8
Bednar, Filip; Schofield, Heather K; Collins, Meredith A et al. (2015) Bmi1 is required for the initiation of pancreatic cancer through an Ink4a-independent mechanism. Carcinogenesis 36:730-8
Wu, Linwei; Nguyen, Liem H; Zhou, Kejin et al. (2015) Precise let-7 expression levels balance organ regeneration against tumor suppression. Elife 4:e09431
Mich, John K; Signer, Robert Aj; Nakada, Daisuke et al. (2014) Prospective identification of functionally distinct stem cells and neurosphere-initiating cells in adult mouse forebrain. Elife 3:e02669
Burgess, R J; Agathocleous, M; Morrison, S J (2014) Metabolic regulation of stem cell function. J Intern Med 276:12-24
Signer, Robert A J; Magee, Jeffrey A; Salic, Adrian et al. (2014) Haematopoietic stem cells require a highly regulated protein synthesis rate. Nature 509:49-54

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