Abstract

Brain injury is a common and untreatable occurrence. Recently, however neurogenesis has been found in the adult mammalian brain. Much of the adult neurogenesis occurs in the subventricular zone (SVZ). The SVZ is a layer of mitotically active neuroblasts, glia, and progenitor cells that flank the lateral ventricles. SVZ cells have stem cell-like properties; when cultured in vitro they are capable of dividing indefinitely, and of differentiating into multiple cell types. The response of the SVZ to brain injury is poorly understood and understudied. These experiments will determine whether aspiration lesions of the sensorimotor cortex in mice, increase cell numbers, change the phenotype, change lineal fate restriction, or induce migration of cells out the SVZ and towards the site of lesion.
Our Aim are: 1. To determine whether cortical lesions change the number of subventricular zone cells and/or the phenotype of newborn SVZ cells in adult mice. Cell numbers and BrdU incorporation will be quantified after unilateral aspiration lesions of the sensorimotor cortex in adult mice and compared to non-lesioned controls. Double immunofluorescence labeling for BrdU and phenotypic markers of cells in the SVZ will be analyzed with confocal microscopy to ascertain the identity of new-born cells after lesions. 2. To determine whether the fate restriction of cells in the SVZ changes after cortical lesions. We will infect SVZ cells with a replication incompetent retroviral library of degenerate oligonucleotides (BOLAP). The phenotypic restriction of clones will be determined with double immunofluorescence for viral epitopes and cell markers. Retrovirally labeled cells will be microdissected and their oligonucleotide inserts sequenced in order to serve as molecular tags of clonal identity. 3. To test the hypothesis that cortical lesions induce migration of cells out of the SVZ toward the lesion. BOLAP or DiI will be injected via ultrasound guidance directly into the SVZ or stereotactically into the lateral ventricle. We will analyze migration out of the SVZ towards the lesioned cortex. If cells migrate out of the SVZ then their phenotype will be ascertained by morphology and phenotype cell marker expression. In addition, structures immediately adjacent to the SVZ will be investigated for the re- emergence of radial glia-like fibers.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS042253-01
Application #
6360298
Study Section
Special Emphasis Panel (ZRG1-BDCN-2 (01))
Program Officer
Michel, Mary E
Project Start
2001-08-01
Project End
2005-07-31
Budget Start
2001-08-01
Budget End
2002-07-31
Support Year
1
Fiscal Year
2001
Total Cost
$201,324
Indirect Cost

  Institution

Name
Children's Memorial Hospital (Chicago)
Department
Type
DUNS #
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Turnquist, Casmir; Wang, Yihua; Severson, David T et al. (2014) STAT1-induced ASPP2 transcription identifies a link between neuroinflammation, cell polarity, and tumor suppression. Proc Natl Acad Sci U S A 111:9834-9
Young, Christopher C; Al-Dalahmah, Osama; Lewis, Nicola J et al. (2014) Blocked angiogenesis in Galectin-3 null mice does not alter cellular and behavioral recovery after middle cerebral artery occlusion stroke. Neurobiol Dis 63:155-64
Young, Christopher C; van der Harg, Judith M; Lewis, Nicola J et al. (2013) Ependymal ciliary dysfunction and reactive astrocytosis in a reorganized subventricular zone after stroke. Cereb Cortex 23:647-59
Comte, Isabelle; Kim, Yongsoo; Young, Christopher C et al. (2011) Galectin-3 maintains cell motility from the subventricular zone to the olfactory bulb. J Cell Sci 124:2438-47
Young, Christopher C; Brooks, Keith J; Buchan, Alastair M et al. (2011) Cellular and molecular determinants of stroke-induced changes in subventricular zone cell migration. Antioxid Redox Signal 14:1877-88
Kim, Yongsoo; Wang, Wei-Zhi; Comte, Isabelle et al. (2010) Dopamine stimulation of postnatal murine subventricular zone neurogenesis via the D3 receptor. J Neurochem 114:750-60
Nie, Kai; Molnar, Zoltan; Szele, Francis G (2010) Proliferation but not migration is associated with blood vessels during development of the rostral migratory stream. Dev Neurosci 32:163-72
Kim, Yongsoo; Comte, Isabelle; Szabo, Gabor et al. (2009) Adult mouse subventricular zone stem and progenitor cells are sessile and epidermal growth factor receptor negatively regulates neuroblast migration. PLoS One 4:e8122
Goings, Gwendolyn E; Greisman, Adriana; James, Rachel E et al. (2008) Hematopoietic cell activation in the subventricular zone after Theiler's virus infection. J Neuroinflammation 5:44
Kim, Yongsoo; Szele, Francis G (2008) Activation of subventricular zone stem cells after neuronal injury. Cell Tissue Res 331:337-45

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