4.8 Article

In Situ implantable, post-trauma microenvironment-responsive, ROS Depletion Hydrogels for the treatment of Traumatic brain injury

Journal

BIOMATERIALS
Volume 270, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2021.120675

Keywords

Traumatic brain injury; Injectable hydrogel; ROS scavengers; Neuron recovery

Funding

  1. National Natural Science Foundation of China [81772665]
  2. Key Research & Development Plan of Jiangsu Province [BE2020647]
  3. Six Talents Peak Foundation of Jiangsu Province [2018WSW-071]
  4. Youth Science and Technology Innovation Team Cultivation Program of Xuzhou Medical University
  5. Key Research & Development Plan of Xuzhou [KC20079]

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A hydrogel embedded with curcumin was developed to reduce excess reactive oxygen species in damaged brain tissue, promoting neuron regeneration and recovery. The hydrogel effectively responded to the traumatic brain injury surgical environment, depleting ROS levels and reducing brain edema while promoting nerve regeneration with strong anti-inflammatory effects.
Traumatic brain injury (TBI) generates excess reactive oxygen species (ROS), which can exacerbate secondary injury and result in disability and death. Secondary injury cascades can trigger the release of uncontrolled ROS into the surrounding normal brain tissue, forming an extended pool of ROS, which leads to massive neuronal death. Here, we developed an injectable, post-trauma microenvironment-responsive, ROS depletion hydrogel embedded curcumin (Cur) (TM/PC) for reducing ROS levels in damaged brain tissue to promote the regeneration and recovery of neurons. Hydrogel was composed of three parts: (1) Hydrophobic poly (propylene sulfide)120 (PPS120) was synthesized, with a ROS quencher and H2O2-responsive abilities, to embed Cur. (2) Matrix metalloproteinase (MMP)-responsive triglycerol monostearate (TM) was used to cover the PPS120 to form a TM/ P hydrogel. (3) Cur could further eradicate the ROS, promoting the regeneration and recovery of neurons. In two postoperative TBI models, TM/PC hydrogel effectively responded the TBI surgical environment and released drug. TM/PC hydrogel significantly depleted ROS and reduced brain edema. In addition, reactive astrocytes and activated microglia were decreased, growth-associated protein 43 (GAP43) and doublecortin (DCX) were increased, suggested that TM/PC hydrogel had the strongest anti-inflammatory effect and effectively promoted nerve regeneration after TBI. This study provides new information for the management of TBI to prevent the secondary spread of damage.

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