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BMSC-Derived Exosomes Carrying miR-26a-5p Ameliorate Spinal Cord Injury via Negatively Regulating EZH2 and Activating the BDNF-TrkB-CREB Signaling
Bone marrow stem cell exosomes with miR-26a-5p may improve spinal cord injury by reducing EZH2 and activating the BDNF-TrkB-CREB pathway
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Abstract
BMSC-derived exosomes carrying miR-26a-5p improved cell proliferation and reduced apoptosis in LPS-treated PC12 cells.
- Exosomes from bone marrow stem cells promoted recovery from spinal cord injury.
- miR-26a-5p delivered by these exosomes directly inhibited the expression of EZH2.
- Inhibition of EZH2 led to increased expression of BDNF, a key factor for neuronal survival.
- Activation of CREB was associated with enhanced transcription of KCC2, which is important for neuronal function.
- Knockdown of miR-26a-5p negated the protective effects of BMSC-derived exosomes, but this was restored through KCC2 overexpression.
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