4.7 Article

Surface-Modified Polypyrrole-Coated PLCL and PLGA Nerve Guide Conduits Fabricated by 3D Printing and Electrospinning

Journal

BIOMACROMOLECULES
Volume -, Issue -, Pages -

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.biomac.2c00626

Keywords

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Funding

  1. Royal Golden Jubilee
  2. National Research University Project (NRU)
  3. Program Management Unit for Human Resources & Institutional Development, Research and Innovation, Office of National Higher Education Science Research and Innovation Policy Council (NXPO) [B16F640001]
  4. Fundamental Fund 2022, Chiang Mai University
  5. Center of Excellence in Materials Science and Technology, Chiang Mai University
  6. National Electronics and Computer Technology Center (NECTEC) , NSTDA
  7. European Union [871650]
  8. Marie Curie Actions (MSCA) [871650] Funding Source: Marie Curie Actions (MSCA)

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By combining 3D printing and electrospinning techniques, PLCL-3D/E and PLGA-3D/E scaffolds with an ideal pore structure for nerve guide conduits were designed. PPy was deposited on the surface of the scaffolds to enhance biocompatibility and conductivity. PLGA-3D/E/PPy showed superior cytocompatibility compared to PLCL-3D/E/PPy.
The efficiency of nerve guide conduits (NGCs) in repairing peripheral nerve injury is not high enough yet to be a substitute for autografts and is still insufficient for clinical use. To improve this efficiency, 3D electrospun scaffolds (3D/E) of poly(L- lactide-co-epsilon-caprolactone) (PLCL) and poly(L-lactide-co-glycolide) (PLGA) were designed and fabricated by the combination of 3D printing and electrospinning techniques, resulting in an ideal porous architecture for NGCs. Polypyrrole (PPy) was deposited on PLCL and PLGA scaffolds to enhance biocompatibility for nerve recovery. The designed pore architecture of these PLCL3D/E and PLGA-3D/E scaffolds exhibited a combination of nano-and microscale structures. The mean pore size of PLCL-3D/ E and PLGA-3D/E scaffolds were 289 +/- 79 and 287 +/- 95 nm, respectively, which meets the required pore size for NGCs. Furthermore, the addition of PPy on the surfaces of both PLCL-3D/E (PLCL-3D/E/PPy) and PLGA-3D/E (PLGA-3D/E/PPy) led to an increase in their hydrophilicity, conductivity, and noncytotoxicity compared to noncoated PPy scaffolds. Both PLCL-3D/E/PPy and PLGA-3D/E/PPy showed conductivity maintained at 12.40 +/- 0.12 and 10.50 +/- 0.08 Scm-1 for up to 15 and 9 weeks, respectively, which are adequate for the electroconduction of neuron cells. Notably, the PLGA-3D/E/PPy scaffold showed superior cytocompatibility when compared with PLCL-3D/E/PPy, as evident via the viability assay, proliferation, and attachment of L929 and SC cells. Furthermore, analysis of cell health through membrane leakage and apoptotic indices showed that the 3D/E/PPy scaffolds displayed significant decreases in membrane leakage and reductions in necrotic tissue. Our finding suggests that these 3D/E/PPy scaffolds have a favorable design architecture and biocompatibility with potential for use in peripheral nerve regeneration applications.

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