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FK506 Protects Neurons Following Peripheral Nerve Injury Via Immunosuppression

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Abstract

In this study, we have evaluated neuroprotective effect of an immunosuppressant immunophilin ligand, FK506, in the sciatic nerve injury model in rats. FK506 was injected to the sciatic nerve transected 3-month-old female Wistar rats (2 mg/kg/day starting 1 day prior to sciatic nerve injury up to 7 day post operation). Equal number of sciatic nerve transected animals served as injured untreated controls. The contralateral side served as respective control. L4-L5 region of the spinal cord was removed on day 1, 3, 7, 14, 21, and 28, post operation and then processed for cryo-sectioning and paraffin sectioning. The cryocut sections were used for immunohistochemistry for localizing all microglia (using anti-Iba-1) and MHC-II expressing microglia (with OX-6). The physical dissector method was applied on Nissl stained paraffin sections for absolute motor neuron counting in the L4-L5 region of spinal cord. FK506 treated animals presented 88.7% neuronal survival while the injured alone had 79.12%, which is significantly less than the treated animals. FK506 caused early proliferation of microglia at 1 and 3 days post operation. FK506 also significantly restricted transformation of these cells in to phagocytes. Colocalization of activated microglia by anti-Iba-1 and OX-6 antibodies, confirms that the MHC-II expressing cells in injured spinal cord are none other than microglial cells and MHC-II expressing cells are significantly less in treated as compared to untreated injured animals. We propose that immunosuppression is one of the main mechanisms by which FK506 protects the central neurons following peripheral injury.

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Acknowledgments

We are thankful to the Department of Science and Technology, Ministry of Science and Technology, for providing financial assistance to carry out this study. We are also thankful to Dr. Y. Imai (National Institute of Neuroscience, Tokyo, Japan) for the generous gift of anti-Iba-1 antibody. In this work facilities generated through the Department of Biotechnology (DBT), Ministry of Science and Technology, assistance to the School of Studies in Neuroscience, Jiwaji University, Gwalior, were also used.

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Correspondence to Kapil Saxena.

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Saxena, K., Patro, N. & Patro, I. FK506 Protects Neurons Following Peripheral Nerve Injury Via Immunosuppression. Cell Mol Neurobiol 27, 1049–1057 (2007). https://doi.org/10.1007/s10571-007-9221-6

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  • DOI: https://doi.org/10.1007/s10571-007-9221-6

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