Abstract

Neural stem cells (NSCs) play critical roles in generating neurons and glia during both embryonic development and adult life. Aberrant NSC behavior could lead to neurological disorders, especially those with developmental etiology, and brain tumors. Drosophila neuroblast provides an excellent model for understanding fundamental aspects of NSC regulation in vivo. The long-term goal of this proposal is to elucidate mechanisms regulating the self-renewal and differentiation of NSCs through combined cell biological, genetic, and molecular analyses. Drosophila neuroblasts undergo stem cell-like self-renewing asymmetric divisions. In each division, one daughter cell remains as a stem cell while the other is committed to differentiation. Factors controlling stem cell self-renewal and differentiation are distributed in a polarized fashion and the mitotic spindles are oriented with respect to this polarity axis, ensuring proper segregation of these important factors between the two daughter cells. Numb is such a factor that is segregated to the differentiating daughter cell during neuroblast division, where it inhibits the renewal of neuroblast cell fate. The asymmetric segregation of Numb requires Partner of Numb (Pon). In the last four years we have focused on identifying molecules that impinge on Pon to regulate Numb and those that regulate mitotic spindle orientation. We have learned that a number of mitotic kinases directly act on Pon and Numb. This raises the interesting possibility that during NSC asymmetric division, a series of mitotic kinases act in concert to ensure the faithful segregation of key cell fate determinants to the appropriate daughter cells. We propose to test this hypothesis. We have also learned that a number of tumor suppressors and kinases are involved in regulating mitotic spindle orientation. We propose to investigate the biochemical and genetic relationships between these signaling molecules and to place them into a pathway. We also propose to assess the contribution of the Pon/Numb pathway and the spindle orientation pathway in controlling NSC self-renewal and to identify new players involved in this process. Given the evolutionary conservation of the molecules studied in this proposal and the conservation of mechanisms underlying NSC asymmetric division, knowledge to be gained from this study shall provide important insights into the understanding of mammalian NSC regulation in vivo and ultimately treating diseases originated from dysfunctional NSCs. PUBLIC HEALTH REVELANCE: Neural stem cells are multi-potent cells that generate the diverse cell types in our brain. The goal of this proposal is to achieve a mechanistic understanding of the basic properties of these special cells and how disease may arise when neural stem cells behave abnormally. Accomplishment of the proposed aims will ultimately help understand and treat a number of neurological disorders originated from aberrant neural stem cells, such as neurodegenerative diseases and brain tumors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS043167-09
Application #
7903430
Study Section
Neurogenesis and Cell Fate Study Section (NCF)
Program Officer
Owens, David F
Project Start
2002-04-01
Project End
2012-03-31
Budget Start
2010-04-01
Budget End
2011-03-31
Support Year
9
Fiscal Year
2010
Total Cost
$346,501
Indirect Cost

  Institution

Name
Stanford University
Department
Pathology
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Gehrke, Stephan; Wu, Zhihao; Klinkenberg, Michael et al. (2015) PINK1 and Parkin control localized translation of respiratory chain component mRNAs on mitochondria outer membrane. Cell Metab 21:95-108
Lee, Kyu-Sun; Wu, Zhihao; Song, Yan et al. (2013) Roles of PINK1, mTORC2, and mitochondria in preserving brain tumor-forming stem cells in a noncanonical Notch signaling pathway. Genes Dev 27:2642-7
Song, Yan; Lu, Bingwei (2012) Interaction of Notch signaling modulator Numb with ?-Adaptin regulates endocytosis of Notch pathway components and cell fate determination of neural stem cells. J Biol Chem 287:17716-28
Ouyang, Yingshi; Petritsch, Claudia; Wen, Hong et al. (2011) Dronc caspase exerts a non-apoptotic function to restrain phospho-Numb-induced ectopic neuroblast formation in Drosophila. Development 138:2185-96
King, Ian; Tsai, Linus T-Y; Pflanz, Ralf et al. (2011) Drosophila tao controls mushroom body development and ethanol-stimulated behavior through par-1. J Neurosci 31:1139-48
Ouyang, Yingshi; Song, Yan; Lu, Bingwei (2011) dp53 Restrains ectopic neural stem cell formation in the Drosophila brain in a non-apoptotic mechanism involving Archipelago and cyclin E. PLoS One 6:e28098
Song, Yan; Lu, Bingwei (2011) Regulation of cell growth by Notch signaling and its differential requirement in normal vs. tumor-forming stem cells in Drosophila. Genes Dev 25:2644-58
Harumoto, Toshiyuki; Ito, Masayoshi; Shimada, Yuko et al. (2010) Atypical cadherins Dachsous and Fat control dynamics of noncentrosomal microtubules in planar cell polarity. Dev Cell 19:389-401
Lu, Bingwei (2009) Recent advances in using Drosophila to model neurodegenerative diseases. Apoptosis 14:1008-20
Lu, Bingwei; Vogel, Hannes (2009) Drosophila models of neurodegenerative diseases. Annu Rev Pathol 4:315-42

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