4.8 Article

Developmentally engineered bio-assemblies releasing neurotrophic exosomes guide in situ neuroplasticity following spinal cord injury

期刊

MATERIALS TODAY BIO
卷 16, 期 -, 页码 -

出版社

ELSEVIER
DOI: 10.1016/j.mtbio.2022.100406

关键词

Bio-assemblies; Exosome; Developmentally engineered; Neuroplasticity; Spinal cord injury

资金

  1. National Natural Science Foundation of China [81970915]
  2. Thousand Talents Plan of Shaanxi Province
  3. Natural Science Fund of Shaanxi for distinguished Young Scholars [2020JC33]
  4. Natural Science Basic Research Plan in Shaanxi Province of China [2020JQ-092]
  5. Key R&D program of Shaanxi Province [2019KW-074, 2021SF-033]
  6. Young Talent Support Plan of Xi'an Jiaotong University

向作者/读者索取更多资源

The emerging tissue-engineered bio-assemblies are revolutionizing regenerative medicine by providing a potential program to support the clinical translation of stem-cell-derived treatments. By using a developmentally engineered strategy, mesenchymal stem cells (MSC) can be assembled into a bio-assembly called Spinor, which promotes the treatment of spinal cord injury by promoting axonal regeneration and supporting the neuroplasticity of the spinal cord in vivo.
The emerging tissue-engineered bio-assemblies are revolutionizing the regenerative medicine, and provide a potential program to guarantee predictive performance of stem-cell-derived treatments in vivo and hence support their clinical translation. Mesenchymal stem cell (MSC) showed the attractive potential for the therapy of nervous system injuries, especially spinal cord injury (SCI), and yet failed to make an impact on clinical outcomes. Herein, under the guidance of the embryonic development theory that appropriate cellular coarctations or clustering are pivotal initiators for the formation of geometric and functional tissue structures, a developmentally engineered strategy was established to assemble DPMSCs into a bio-assembly termed Spinor through a three-level sequential induction programme including reductant, energy and mechanical force stimulation. Spinor exhibited similar geometric construction with spinal cord tissue and attain autonomy to released exosome with the optimized quantity and quality for suppressing cicatrization and inflammation and promoting axonal regeneration. As a spinal cord fascia and exosome mothership, Spinor guided the in-situ neuroplasticity of spinal cord in vivo, and caused the significant motor improvement, sensory recovery, and faster urinary reflex restoration in rats following SCI, while maintaining a highly favorable biosafety profile. Collectively, Spinor not only is a potentially clinical therapeutic paradigm as a living exosome mothership for revisiting Prometheus' Myth in SCI, but can be viewed allowing developmentally engineered manufacturing of biomimetic bio-assemblies with complex topology features and inbuilt biofunction attributes towards the regeneration of complex tissues including nervous system.

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