4.7 Article

Sustained-release of FGF-2 from a hybrid hydrogel of heparin-poloxamer and decellular matrix promotes the neuroprotective effects of proteins after spinal injury

Journal

INTERNATIONAL JOURNAL OF NANOMEDICINE
Volume 13, Issue -, Pages 681-694

Publisher

DOVE MEDICAL PRESS LTD
DOI: 10.2147/IJN.S152246

Keywords

spinal cord injury; decellularized extracellular matrix; thermosensitive hydrogel; adsorption; basic fibroblast growth factor

Funding

  1. National Natural Science Foundation of China [81571392, 81603036, 81360195, 81772316]
  2. Key Research and Development Program of Zhejiang Province [2018C03013]
  3. Zhejiang Provincial Program for the Cultivation of High-level Innovative Health Talents
  4. 151 Talent Project of Zhejiang Province
  5. 551 Talent Project of Wenzhou
  6. Key Support of High-level Talent Innovation and Technology project of Wenzhou
  7. School Talent Start Fund of Wenzhou Medical University [QTJ15020]

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Introduction: The short lifetime of protein-based therapies has largely limited their therapeutic efficacy in injured nervous post-spinal cord injury (post-SCI). Methods: In this study, an affinity-based hydrogel delivery system provided sustained-release of proteins, thereby extending the efficacy of such therapies. The affinity-based hydrogel was constructed using a novel polymer, heparin-poloxamer (HP), as a temperature-sensitive bulk matrix and decellular spinal cord extracellular matrix (dscECM) as an affinity depot of drug. By tuning the concentration of HP in formulation, the cold ternary fibroblast growth factor-2 (FGF2)-dscECM-HP solution could rapidly gelatinize into a hydrogel at body temperature. Due to the strong affinity for FGF2, hybrid FGF2-dscECM-HP hydrogel enabled sustained-release of encapsulated FGF2 over an extended period in vitro. Results: Compared to free FGF2, it was observed that both neuron functions and tissue morphology after SCI were clearly recovered in rats treated with FGF2-dscECM-HP hydrogel. Moreover, the expression of neurofilament protein and the density of axons were increased after treatment with hybrid FGF2-dscECM-HP. In addition, the neuroprotective effects of FGF2-dscECM-HP were related to inhibition of chronic endoplasmic reticulum stress-induced apoptosis. Conclusion: The results revealed that a hybrid hydrogel system may be a potential carrier to deliver macromolecular proteins to the injured site and enhance the therapeutic effects of proteins.

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