Abstract

? ? Permanent demyelination, the major pathology of multiple sclerosis, involves the disruption of axonal myelin, impairment of impulse transmission and neuronal damage. It is of therapeutic importance to re-populate the lesions with oligodendrocyte progenitors capable of differentiating and remyelinating damaged neurons. In the postnatal brain, mature oligodendrocytes originate from subventricular zone (SVZ) oligodendrocyte progenitor cells (OPCs), which express the proteoglycan NG2. The molecular signals that regulate OPC development and oligodendrocyte regeneration are still poorly defined. We have recently analyzed OPC migration in vitro and in vivo, and used a CNP-hEGFR mouse, in which all NG2+ OPCs overexpress the hEGFR, to demonstrate that EGFR plays a crucial role in supporting NG2+ cell migration to different brain regions, including the subcortical white matter. A preliminary analysis of the postnatal SVZ in the CNP- hEGFR mouse showed that overexpression of the EGFR stimulates proliferation of NG2+ progenitors and expands the endogenous pool of these cells. These expanded SVZ NG2+ cells also express the transcription factors Mashl and Olig2, and generate oligodendrocytes in vitro. We propose to use the CNP- hEGFR mouse to further define the developmental properties of NG2+Mash1+Olig2+ progenitors in the postnatal SVZ and to characterize their participation in oligodendrogenesis. We will then compare white matter development and myelination in the CNP-hEGFR with that in wild type (wt) mice. Finally, we will compare the regenerative and remyelinating potential of NG2+Mash1+Olig2+ progenitors from CNP-hEGFR mice with their wt counterpart in two animal models of demyelination- lysolecithin-induced focal demyelination and cuprizone-induced generalized demyelination. These analyses will reveal important roles for EGFR in neural progenitor cell proliferation and migration in the postnatal brain, and will offer new avenues to improve oligodendrocyte regeneration from neural progenitor after demyelination. Our proposed studies aim to shed light on crucial regulators of oligodendrocyte development and remyelination that are potentially useful in therapeutic strategies. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Career Transition Award (K99)
Project #
1K99NS057944-01
Application #
7224077
Study Section
Special Emphasis Panel (ZNS1-SRB-M (38))
Program Officer
Utz, Ursula
Project Start
2007-06-01
Project End
2009-05-31
Budget Start
2007-06-01
Budget End
2008-05-31
Support Year
1
Fiscal Year
2007
Total Cost
$88,113
Indirect Cost

  Institution

Name
Children's Research Institute
Department
Type
DUNS #
143983562
City
Washington
State
DC
Country
United States
Zip Code
20010

  Publications

Birey, Fikri; Aguirre, Adan (2015) Age-Dependent Netrin-1 Signaling Regulates NG2+ Glial Cell Spatial Homeostasis in Normal Adult Gray Matter. J Neurosci 35:6946-51
Aguirre, Adan; Rubio, Maria E; Gallo, Vittorio (2010) Notch and EGFR pathway interaction regulates neural stem cell number and self-renewal. Nature 467:323-7
Jablonska, Beata; Aguirre, Adan; Raymond, Matthew et al. (2010) Chordin-induced lineage plasticity of adult SVZ neuroblasts after demyelination. Nat Neurosci 13:541-550
Etxeberria, Ainhoa; Mangin, Jean-Marie; Aguirre, Adan et al. (2010) Adult-born SVZ progenitors receive transient synapses during remyelination in corpus callosum. Nat Neurosci 13:287-289
Li, Xuekun; Tang, Xiaobing; Jablonska, Beata et al. (2009) p27(KIP1) regulates neurogenesis in the rostral migratory stream and olfactory bulb of the postnatal mouse. J Neurosci 29:2902-14
Gadea, Ana; Aguirre, Adan; Haydar, Tarik F et al. (2009) Endothelin-1 regulates oligodendrocyte development. J Neurosci 29:10047-62