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Human neural stem cells improve sensorimotor deficits in the adult rat brain with experimental focal ischemia.

作者信息

Chu Kon, Kim Manho, Park Kyung-Il, Jeong Sang-Wuk, Park Hee-Kwon, Jung Keun-Hwa, Lee Soon-Tae, Kang Lami, Lee Kyungmi, Park Dong-Kyu, Kim Seung U, Roh Jae-Kyu

机构信息

Department of Neurology, Stroke and Neural Stem Cell Laboratory in Clinical Research Institute, Seoul National University Hospital, Seoul National University, 28, Yongon-Dong, Chongro-Gu, Seoul 110-744, South Korea.

出版信息

Brain Res. 2004 Aug 6;1016(2):145-53. doi: 10.1016/j.brainres.2004.04.038.


DOI:10.1016/j.brainres.2004.04.038
PMID:15246850
Abstract

Ischemic stroke is caused by the interruption of cerebral blood flow that leads to brain damage with long-term sensorimotor deficits. Stem cell transplantation may recover functional deficit by replacing damaged brain. In this study, we attempted to test whether the human neural stem cells (NSCs) can improve the outcome in the rat brain with intravenous injection and also determine the migration, differentiation and the long-term viabilities of human NSCs in the rat brain. Focal cerebral ischemia was induced by intraluminal thread occlusion of middle cerebral artery (MCA). One day after surgery, the rats were randomly divided into two groups: NSCs-ischemia vs. Ischemia-only. Human NSCs infected with retroviral vector encoding beta galactosidase were intravenously injected in NSCs-ischemia group (5 x 10(6) cells) and the same amount of saline was injected in Ischemia-only group for control. The animals were evaluated for 4 weeks using turning in an alley (TIA) test, modified limb placing test (MLPT) and rotarod test. Transplanted cells were detected by X gal cytohistochemistry or beta gal immunohistochemistry with double labeling of other cell markers. The NSCs-ischemia group showed better performance on TIA test at 2 weeks, and MLPT and rotarod test from 3 weeks after ischemia compared with the Ischemia-only group. Human NSCs were detected in the lesion side and labeled with marker for neurons or astrocytes. Postischemic hemispheric atrophy was noted but reduced in NSCs-ischemia group. X gal+ cells were detected in the rat brain as long as 540 days after transplantation. Our data suggest intravenously transplanted human NSCs can migrate and differentiate in the rat brain with focal ischemia and improve functional recovery.

摘要

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[2]
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Stem Cell Rev Rep. 2024-4

[3]
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Neuroprotection. 2023-12

[4]
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[5]
Editing a gateway for cell therapy across the blood-brain barrier.

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[6]
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[7]
Neural Stem Cells for Early Ischemic Stroke.

Int J Mol Sci. 2021-7-19

[8]
Reliable generation of glial enriched progenitors from human fibroblast-derived iPSCs.

Stem Cell Res. 2021-8

[9]
Insight Into the Mechanisms and the Challenges on Stem Cell-Based Therapies for Cerebral Ischemic Stroke.

Front Cell Neurosci. 2021-2-25

[10]
Therapeutic Plasticity of Neural Stem Cells.

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