4.7 Article

Gene delivery of chitosan-graft-polyethyleneimine vectors loaded on scaffolds for nerve regeneration

Journal

CARBOHYDRATE POLYMERS
Volume 290, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.carbpol.2022.119499

Keywords

Chitosan; graft -polyethyleneimine; Gene therapy; C-Jun; Nerve factors; Nerve regeneration

Funding

  1. National key research and devel-opment program of China [2018YFC1106800]
  2. Sichuan Science and Technology Project [2018JY0535]
  3. Chongqing Talents Project [CQYC202105043]
  4. Talents Training Program of Army Medical University [2019MPRC021/SWH2018QNWQ-05]

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By constructing gene vectors and nerve scaffolds, successful localized delivery of c-Jun plasmids and upregulation of nerve growth factor expression were achieved, promoting nerve regeneration and functional recovery.
As an important transcription factor, c-Jun could upregulate growth factors expression in Schwann cells (SCs). Arginine-Glycine-Aspartate (RGD)-functionalized chitosan-graft-polyethyleneimine (RCP) gene vectors were prepared through the maleic anhydride & the carbodiimide methods, and electrostatically bound with c-Jun plasmids (pJUN), finally loaded on poly-L-lactic acid/silk fibroin parallel fiber films to fabricate nerve scaffold (RCP/pJUN-PSPF@PGA), which could locally deliver c-Jun plasmids into SCs via the mediation of RGD peptides, and upregulate the expression of nerve growth factor (NGF) and brain-derived neurotrophic factor (BDNF) in SCs. After the scaffold was bridged in sciatic nerve defect, the delivery of c-Jun plasmids from RCP/pJUNPSPF@PGA facilitated SCs to sustain the expressions of NGF, BDNF and vascular endothelial growth factor in the injury field, promoting myelination, axonal growth and microvascular generation and nerve regeneration, muscle reinnervation and functional recovery. These results suggested that RCP/pDNA-PSPF@PGA, as an effective gene delivery platform, could provide a local gene therapy to improve nerve regeneration.

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