Injectable multifunctional scaffold for spinal cord repair

Spinal cord injury (SCI) affects thousands of Americans each year. The injury results in local cell loss in the spinal cord, interrupting the connections between brain and periphery. Current treatment options for SCI are limited due to the inability of adult neurons to regenerate in the inhibitory e...

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Bibliographic Details
Published inProceedings of the 2010 IEEE 36th Annual Northeast Bioengineering Conference (NEBEC) pp. 1 - 2
Main Authors Conova, Lauren, Kubinski, Pamela, Ying Jin, Vernengo, Jennifer, Neuhuber, Birgit, Fischer, Itzhak, Lowman, Anthony
Format Conference Proceeding
LanguageEnglish
Published IEEE 01.03.2010
Subjects
Central nervous system
Chemical engineering
In vitro
In vivo
Nerve fibers
Neurons
Polymer gels
Rodents
Spinal cord
Spinal cord injury
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ISBN9781424468799
1424468795
ISSN2160-6986
DOI10.1109/NEBC.2010.5458269

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Summary:Spinal cord injury (SCI) affects thousands of Americans each year. The injury results in local cell loss in the spinal cord, interrupting the connections between brain and periphery. Current treatment options for SCI are limited due to the inability of adult neurons to regenerate in the inhibitory environment of the injured central nervous system (CNS). The primary goal of this work is to design a multifunctional, injectable hydrogel that supports neural repair following SCI. This project proposes the use of a branched copolymer based on poly(N-isopropylacryalmide) (PNIPAAm) and poly(ethylene glycol) (PEG). The thermosensitive nature of the hydrogel allows for easy implantation together with cellular grafts, and the controlled delivery of therapeutic factors. In this study, we investigated the cytocompatibility of the scaffold in vitro and also report its performance in vivo, with and without brain derived neurotrophic factor (BDNF) in a rodent model of SCI. Our results show that the injectable PNIPAAm-PEG scaffold completely fills the injury site, and does not elicit a larger host inflammatory response than a commercially available gelatin sponge. In addition, we have shown that the scaffold loaded with BDNF is permissive to host axon growth. With these promising results, we suggest that an injectable PNIPAAm-PEG hydrogel can serve as a multifunctional device that will result in an effective platform technology for the treatment of SCI.
ISBN:9781424468799
1424468795
ISSN:2160-6986
DOI:10.1109/NEBC.2010.5458269