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Modulation of Glial and Neuronal Migration by Lipocalin-2 in ZebrafishModulation of Glial and Neuronal Migration by Lipocalin-2 in Zebrafish

Other Titles
Modulation of Glial and Neuronal Migration by Lipocalin-2 in Zebrafish
Authors
김호이명식석경호이신려이원하박해철
Issue Date
2011
Publisher
대한면역학회
Keywords
LCN2; Glia; Cell migration; Neuroinflammation; Central nervous system; Spinal cord
Citation
Immune Network, v.11, no.6, pp.342 - 347
Indexed
KCI
Journal Title
Immune Network
Volume
11
Number
6
Start Page
342
End Page
347
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/113948
ISSN
1598-2629
Abstract
Background: Glial cells are involved in immune and inflammatory responses in the central nervous system (CNS). Glial cells such as microglia and astrocytes also provide structural and functional support for neurons. Migration and morphological changes of CNS cells are associated with their physiological as well as pathological functions. The secreted protein lipocalin-2 (LCN2) has been previously implicated in regulation of diverse cellular processes of glia and neurons, including cell migration and morphology. Methods:Here, we employed a zebrafish model to analyze the role of LCN2 in CNS cell migration and morphology in vivo. In the first part of this study, we examined the indirect effect of LCN2 on cell migration and morphology of microglia, astrocytes,and neurons cultured in vitro. Results: Conditioned media collected from LCN2-treated astrocytes augmented migration of glia and neurons in the Boyden chamber assay. The conditioned media also increased the number of neuronal processes. Next, in order to further understand the role of LCN2 in the CNS in vivo, LCN2 was ectopically expressed in the zebrafish spinal cord. Expression of exogenous LCN2 modulated neuronal cell migration in the spinal cord of zebrafish embryos, supporting the role of LCN2 as a cell migration regulator in the CNS. Conclusion: Thus, LCN2proteins secreted under diverse conditions may play an important role in CNS immune and inflammatory responses by controlling cell migration and morphology.
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