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miR-NPs-RVG promote spinal cord injury repair: implications from spinal cord-derived microvascular endothelial cells

JOURNAL OF NANOBIOTECHNOLOGY [2024]
Li Chao, Xiang Zhenyang, Hou Mengfan, Yu Hao, Peng Peng, Lv Yigang, Ma Chao, Ding Han, Jiang Yunpeng, Liu Yang, Zhou Hengxing, Feng Shiqing
ABSTRACT

Background Spinal cord injury (SCI) often leads to a loss of motor and sensory function. Axon regeneration and outgrowth are key events for functional recovery after spinal cord injury. Endogenous growth of axons is associated with a variety of factors. Inspired by the relationship between developing nerves and blood vessels, we believe spinal cord-derived microvascular endothelial cells (SCMECs) play an important role in axon growth. Results We found SCMECs could promote axon growth when co-cultured with neurons in direct and indirect co-culture systems via downregulating the miR-323-5p expression of neurons. In rats with spinal cord injury, neuron-targeting nanoparticles were employed to regulate miR-323-5p expression in residual neurons and promote function recovery. Conclusions Our study suggests that SCMEC can promote axon outgrowth by downregulating miR-323-5p expression within neurons, and miR-323-5p could be selected as a potential target for spinal cord injury repair. Graphical Abstract

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