Interactome and reciprocal activation of pathways in topical mesenchymal stem cells and the recipient cerebral cortex following traumatic brain injury

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作者
Ping K. Lam
Kevin K. W. Wang
Anthony W. I. Lo
Cindy S. W. Tong
Don W. C. Ching
Kenneth Wong
Zhihui Yang
Themis Kong
Kin K. Y. Lo
Richard K. W. Choy
Paul B. S. Lai
George K. C. Wong
Wai S. Poon
机构
[1] The Chinese University of Hong Kong,Department of Surgery
[2] The Chinese University of Hong Kong,Chow Tai Fook
[3] The Chinese University of Hong Kong,Cheng Yu Tung Surgical Stem Cell Research Center
[4] The Chinese University of Hong Kong,Department of Anatomical & Cellular Pathology
[5] University of Florida,Department of Obstetrics and Gynecology
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In this study, GFP-MSCs were topically applied to the surface of cerebral cortex within 1 hour of experimental TBI. No treatment was given to the control group. Three days after topical application, the MSCs homed to the injured parenchyma and improved the neurological function. Topical MSCs triggered earlier astrocytosis and reactive microglia. TBI penumbra and hippocampus had higher cellular proliferation. Apoptosis was suppressed at hippocampus at 1 week and reduced neuronal damaged was found in the penumbral at day 14 apoptosis. Proteolytic neuronal injury biomarkers (alphaII-spectrin breakdown products, SBDPs) and glial cell injury biomarker, glial fibrillary acidic protein (GFAP)-breakdown product (GBDPs) in injured cortex were also attenuated by MSCs. In the penumbra, six genes related to axongenesis (Erbb2); growth factors (Artn, Ptn); cytokine (IL3); cell cycle (Hdac4); and notch signaling (Hes1) were up-regulated three days after MSC transplant. Transcriptome analysis demonstrated that 7,943 genes were differentially expressed and 94 signaling pathways were activated in the topical MSCs transplanted onto the cortex of brain injured rats with TBI. In conclusion, topical application offers a direct and efficient delivery of MSCs to the brain.
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