4.8 Article

Biopolymer-nanotube nerve guidance conduit drug delivery for peripheral nerve regeneration: In vivo structural and functional assessment

期刊

BIOACTIVE MATERIALS
卷 6, 期 9, 页码 2881-2893

出版社

KEAI PUBLISHING LTD
DOI: 10.1016/j.bioactmat.2021.02.016

关键词

Peripheral nerve regeneration; Nerve guidance conduit; Sciatic nerve transection; Small-molecule drug delivery; Neurotrophic factor; Functional recovery

资金

  1. National Institute of Biomedical Imaging and Bioengineering of the National Institutes of Health [R01EB020640]
  2. Department of Defense through the Peer Reviewed Orthopaedic Research Program [W81XWH-13-1-0320]
  3. National Science Foundation (NSF) Graduate Research Fellowship [DGE-1747453]

向作者/读者索取更多资源

The study investigates novel nerve guidance conduits with aligned microchannel porosity delivering sustained-release of neurogenic 4-aminopyridine for peripheral nerve regeneration. Results show equivalency with autograft controls in terms of functional recovery, myelin development, and histological assessments. The aligned microchannel architecture of the conduit guides axons and the sustained release of 4-AP increases nerve conduction.
Peripheral nerve injuries account for roughly 3% of all trauma patients with over 900,000 repair procedures annually in the US. Of all extremity peripheral nerve injuries, 51% require nerve repair with a transected gap. The current gold-standard treatment for peripheral nerve injuries, autograft repair, has several shortcomings. Engineered constructs are currently only suitable for short gaps or small diameter nerves. Here, we investigate novel nerve guidance conduits with aligned microchannel porosity that deliver sustained-release of neurogenic 4-aminopyridine (4-AP) for peripheral nerve regeneration in a critical-size (15 mm) rat sciatic nerve transection model. The results of functional walking track analysis, morphometric evaluations of myelin development, and histological assessments of various markers confirmed the equivalency of our drug-conduit with autograft controls. Repaired nerves showed formation of thick myelin, presence of 5100 and neurofilament markers, and promising functional recovery. The conduit's aligned microchannel architecture may play a vital role in physically guiding axons for distal target reinnervation, while the sustained release of 4-AP may increase nerve conduction, and in turn synaptic neurotransmitter release and upregulation of critical Schwann cell neurotrophic factors. Overall, our nerve construct design facilitates efficient and efficacious peripheral nerve regeneration via a drug delivery system that is feasible for clinical applications.

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