4.7 Article

Polydatin protects Schwann cells from methylglyoxal induced cytotoxicity and promotes crushed sciatic nerves regeneration of diabetic rats

Journal

PHYTOTHERAPY RESEARCH
Volume 35, Issue 8, Pages 4592-4604

Publisher

WILEY
DOI: 10.1002/ptr.7177

Keywords

diabetic sciatic nerves damage; neuroprotective effects; oxidative stress; polydatin; Schwann cells

Funding

  1. National Natural Science Foundation of China [81571921, 81671908]

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Our study demonstrated that PD has notable neuroprotective effects on Schwann cells and sciatic nerves in diabetic models, potentially through activating Nrf2 and GLO1, which opens up new possibilities for treating diabetic peripheral neuropathy.
Oxidative stress plays the main role in the pathogenesis of diabetes mellitus and peripheral neuropathy. Polydatin (PD) has been shown to exhibit strong antioxidative and antiinflammatory effects. At present, no research has focused on the possible effects of PD on Schwann cells and impaired peripheral nerves in diabetic models. Here, we used an in vitro Schwann cell damage model induced by methylglyoxal and an in vivo diabetic sciatic nerve crush model to study problems in such an area. In our experiment, we demonstrated that PD potently alleviated the decrease of cellular viability, prevented reactive oxygen species generation, and suppressed mitochondrial depolarization as well as cellular apoptosis in damaged Schwann cells. Moreover, we found that PD could upregulate Nrf2 and Glyoxalase 1 (GLO1) expression and inhibit Keap1 and receptor of AGEs (RAGE) expression of damaged Schwann cells. Finally, our in vivo experiment showed that PD could promote sciatic nerves repair of diabetic rats. Our results revealed that PD exhibited prominent neuroprotective effects on Schwann cells and sciatic nerves in diabetic models. The molecular mechanisms were associated with activating Nfr2 and GLO1 and inhibiting Keap1 and RAGE.

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