1. Neural stem cell small extracellular vesicle-based delivery of 14-3-3t reduces apoptosis and neuroinflammation following traumatic spinal cord injury by enhancing autophagy by targeting Beclin-1
- Author
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Weihua Cai, Qingqing Li, Chengtang Lv, Guoyong Yin, Jiaxing Wang, Dongdong Jiang, Wei Zhou, Wei Liu, Zheng Zhou, Linwei Li, Yuluo Rong, Lipeng Yu, Jin Fan, and Yongjun Luo
- Subjects
Autophagosome ,autophagy ,Aging ,viruses ,Apoptosis ,Motor Activity ,14-3-3t ,Rats, Sprague-Dawley ,Extracellular Vesicles ,Mice ,NSC-sEVs ,Neural Stem Cells ,In vivo ,medicine ,Animals ,Spinal cord injury ,Spinal Cord Injuries ,Neuroinflammation ,Neurons ,Gene knockdown ,Chemistry ,Autophagy ,virus diseases ,Recovery of Function ,Cell Biology ,Extracellular vesicle ,respiratory system ,medicine.disease ,spinal cord injury ,Neural stem cell ,Rats ,nervous system diseases ,Cell biology ,14-3-3 Proteins ,nervous system ,Cytokines ,Beclin-1 ,Microglia ,Research Paper - Abstract
Neural stem cell-derived small extracellular vesicles (NSC-sEVs) play an important role in the repair of tissue damage. Our previous in vitro and in vivo studies found that preconditioning with NSC-sEVs promoted the recovery of functional behaviors following spinal cord injury by activating autophagy. However, the underlying mechanisms for such observations remain unclear. In this study, we further explored the mechanisms by which NSC-sEVs repair spinal cord injury via autophagy. We found that NSC-sEVs contain 14-3-3t protein, of which the overexpression or knockdown enhanced and decreased autophagy, respectively. In addition, 14-3-3t overexpression enhanced the anti-apoptotic and anti-inflammatory effects of NSC-sEVs, further promoting functional behavior recovery following spinal cord injury. The overexpression of 14-3-3t was used to further validate the in vivo results through a series of in vitro experiments. Conversely, knockdown of 14-3-3t attenuated the anti-apoptotic and anti-inflammatory effects of NSC-sEVs. Further studies also confirmed that NSC-sEVs increased Beclin-1 expression, with which 14-3-3t interacted and promoted its localization to autophagosome precursors. In this study, we found that NSC-sEVs deliver 14-3-3t, which interacts with Beclin-1 to activate autophagy. Our results indicate that 14-3-3t acts via a newly-discovered mechanism for the activation of autophagy by NSC-sEVs.
- Published
- 2019
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