| Literature DB >> 24412492 |
Mia Emgård1, Jinghua Piao1, Helena Aineskog2, Jia Liu1, Cinzia Calzarossa1, Jenny Odeberg1, Lena Holmberg1, Eva-Britt Samuelsson1, Bartosz Bezubik3, Per Henrik Vincent1, Scott P Falci4, Åke Seiger2, Elisabet Åkesson2, Erik Sundström5.
Abstract
To validate human neural precursor cells (NPCs) as potential donor cells for transplantation therapy after spinal cord injury (SCI), we investigated the effect of NPCs, transplanted as neurospheres, in two different rat SCI models. Human spinal cord-derived NPCs (SC-NPCs) transplanted 9 days after spinal contusion injury enhanced hindlimb recovery, assessed by the BBB locomotor test. In spinal compression injuries, SC-NPCs transplanted immediately or after 1 week, but not 7 weeks after injury, significantly improved hindlimb recovery compared to controls. We could not detect signs of mechanical allodynia in transplanted rats. Four months after transplantation, we found more human cells in the host spinal cord than were transplanted, irrespective of the time of transplantation. There was no focal tumor growth. In all groups the vast majority of NPCs differentiated into astrocytes. Importantly, the number of surviving rat spinal cord neurons was highest in groups transplanted acutely and subacutely, which also showed the best hindlimb function. This suggests that transplanted SC-NPCs improve the functional outcome by a neuroprotective effect. We conclude that SC-NPCs reliably enhance the functional outcome after SCI if transplanted acutely or subacutely, without causing allodynia. This therapeutic effect is mainly the consequence of a neuroprotective effect of the SC-NPCs.Entities:
Keywords: Motor function; Neural precursor cells; Neuroprotection; Spinal cord injury; Transplantation
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Year: 2014 PMID: 24412492 DOI: 10.1016/j.expneurol.2013.12.022
Source DB: PubMed Journal: Exp Neurol ISSN: 0014-4886 Impact factor: 5.330