Cell Proliferation and Neuroblast Differentiation in the Rat Dentate Gyrus After Intrathecal Treatment with Adipose-Derived Mesenchymal Stem Cells

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作者
Jung Hoon Choi
Jin Young Chung
Dae Young Yoo
In Koo Hwang
Ki-Yeon Yoo
Choong Hyun Lee
Bing Chun Yan
Jin Ok Ahn
Hwa Young Youn
Moo-Ho Won
机构
[1] College of Veterinary Medicine,Department of Anatomy
[2] Kangwon National University,Department of Veterinary Internal Medicine
[3] College of Veterinary Medicine,Department of Neurology
[4] Seoul National University,Department of Anatomy and Cell Biology
[5] Clinical Research Institute,Department of Oral Anatomy
[6] Seoul National University Hospital,Department of Neurobiology
[7] College of Veterinary Medicine,undefined
[8] and Research Institute for Veterinary Science,undefined
[9] Seoul National University,undefined
[10] College of Dentistry,undefined
[11] Gangneung-Wonju National University,undefined
[12] School of Medicine,undefined
[13] Kangwon National University,undefined
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关键词
Neurogenesis; Ki67; Doublecortin; Subgranular zone; Hippocampus;
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摘要
Mesenchymal stem cells (MSC) have emerged as a new therapeutic tool for a number of clinical applications, because they have multipotency and paracrine effects via various factors. In the present study, we investigated the effects of adipose-derived MSC (Ad-MSC) transplantation via intrathecal injection through the cisterna magna on cell proliferation and differentiation of endogenous stem cells in the hippocampal dentate gyrus (DG) using Ki-67 (a marker for proliferating cells), and doublecortin (DCX, a marker for neuroblasts). The transplanted Ad-MSC were detected in the meninges, not in the hippocampal parenchyma. However, the number of Ki-67-immunoreactive cells was significantly increased by 83% in the DG 2 days after single Ad-MSC injection, and by 67% at 23 days after repeated Ad-MSC treatment compared with that in the vehicle-treated group after Ad-MSC transplantation. On the other hand, the number of DCX-immunoreactive cells in the DG was not changed at 2 days after single Ad-MSC injection; however, it was significantly increased by 62% 9 days after single Ad-MSC injection. At 23 days after repeated Ad-MSC application, the number of DCX-immunoreactive cells was much more increased (223% of the vehicle-treated group). At this time point, DCX protein levels were also significantly increased compared with those in the vehicle-treated group. These results suggest that the intrathecal injection of Ad-MSC could enhance endogenous cell proliferation, and the repeated Ad-MSC injection could be more efficient for an enhancement of endogenous cell proliferation and differentiation in the brain.
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