Serum response factor promoting axonal regeneration by activating the Ras–Raf‐Cofilin signaling pathway after the spinal cord injury

Author:

Gao Limin12,Zhang Chen13,Zhu Yonglin4,Zhang Naili1,Zhang Chunlei1,Zhou Shuai1,Feng Guoying1,Huang Fei15,Zhang Luping1ORCID

Affiliation:

1. Institute of Neurobiology, Binzhou Medical University Yantai Shandong Province China

2. Department of Neurobiology School of Basic Medical Sciences, Capital Medical University Beijing China

3. Experimental Neurosurgery, Department of Neurosurgery Neuroscience Center, Frankfurt University Hospital Frankfurt am Main Germany

4. Department of Bone and Joint Yantai Affiliated Hospital of Binzhou Medical University Yantai Shandong China

5. University of Health and Rehabilitation Sciences Qingdao Shandong Province China

Abstract

AbstractIntroductionSerum response factor (SRF) is important in muscle development, tissue repair, and neuronal regulation.ObjectivesThis research aims to thoroughly examine the effects of SRF on spinal cord injury (SCI) and its ability to significantly impact the recovery and regeneration of neuronal axons.MethodsThe researchers created rat models of SCI and scratch injury to primary spinal cord neurons to observe the expression of relevant factors after neuronal injury.ResultsWe found that the SRF, Ras, Raf, and cofilin levels increased after injury and gradually returned to normal levels. Afterward, researchers gave rats with SCI an SRF inhibitor (CCG1423) and studied the effects with nuclear magnetic resonance and transmission electron microscopy. The SRF inhibitor rodents had worse spinal cord recovery and axon regrowth than the control group. And the apoptosis of primary neurons after scratch injury was significantly higher in the SRF inhibitor group. Additionally, the researchers utilized lentiviral transfection to modify the SRF expression in neurons. SRF overexpression increased neuron migration while silencing SRF decreased it. Finally, Western blotting and RT‐PCR were conducted to examine the expression changes of related factors upon altering SRF expression. The results revealed SRF overexpression increased Ras, Raf, and cofilin expression. Silencing SRF decreased Ras, Raf, and Cofilin expression.ConclusionBased on our research, the SRF promotes axonal regeneration by activating the “Ras–Raf‐Cofilin” signaling pathway.

Publisher

Wiley

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