AI Article Synopsis

  • Bupivacaine can cause neurotoxicity by increasing reactive oxygen species (ROS), but the exact mechanism involved, particularly the role of the p47phox protein, is not well understood.
  • Researchers conducted in vitro experiments using human neuroblastoma cells and in vivo tests on rats to investigate how inhibiting NOX activity and modifying p47phox levels affect this neurotoxicity.
  • The findings revealed that blocking the membrane translocation of p47phox with a NOX inhibitor (VAS2870) or using p47phox-siRNA reduced the neurotoxic effects of bupivacaine, highlighting p47phox's central role in the process.

Article Abstract

Bupivacaine has been shown to induce neurotoxicity through inducing excessive reactive oxygen species (ROS), but the underlying mechanism remains unclear. NOX2 is one of the most important sources of ROS in the nervous system, and its activation requires the membrane translocation of subunit p47phox. However, the role of p47phox in bupivacaine-induced neurotoxicity has not been explored. In our in vitro study, cultured human SH-SY5Y neuroblastoma cells were treated with 1.5 mM bupivacaine to induce neurotoxicity. Membrane translocation of p47phox was assessed by measuring the cytosol/membrane ratio of p47phox. The effects of the NOX inhibitor VAS2870 and p47phox-siRNA on bupivacaine-induced neurotoxicity were investigated. Furthermore, the effect of VAS2870 on bupivacaine-induced neurotoxicity was assessed in vivo in rats. All these changes were reversed by pretreatment with VAS2870 or transfection with p47phox-siRNA in SH-SY5Y cells. Similarly, pretreatment with VAS2870 attenuated bupivacaine-induced neuronal toxicity in rats. It is concluded that enhancing p47phox membrane translocation is a major mechanism whereby bupivacaine induced neurotoxicity and that pretreatment with VAS2870 or local p47phox gene knockdown attenuated bupivacaine-induced neuronal cell injury.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5480047PMC
http://dx.doi.org/10.1155/2017/8539026DOI Listing

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