| Literature DB >> 27152884 |
Naoko Niimi1, Hideji Yako1, Masami Tsukamoto1,2, Shizuka Takaku1, Junji Yamauchi3, Emiko Kawakami1, Hiroko Yanagisawa1, Kazuhiko Watabe1, Kazunori Utsunomiya2, Kazunori Sango1.
Abstract
Amiodarone hydrochloride (AMD), an anti-arrhythmic agent, has been shown to cause peripheral neuropathy; however, its pathogenesis remains unknown. We examined the toxic effects of AMD on an immortalized adult rat Schwann cell line, IFRS1, and cocultures of IFRS1 cells and adult rat dorsal root ganglion neurons or nerve growth factor-primed PC12 cells. Treatment with AMD (1, 5, and 10 μm) induced time- and dose-dependent cell death, accumulation of phospholipids and neutral lipids, upregulation of the expression of gangliosides, and oxidative stress (increased nuclear factor E2-related factor in nuclear extracts and reduced GSH/GSSG ratios) in IFRS1 cells. It also induced the upregulation of LC3-II and p62 expression, with phosphorylation of p62, suggesting that deficient autolysosomal degradation is involved in AMD-induced IFRS1 cell death. Furthermore, treatment of the cocultures with AMD induced detachment of IFRS1 cells from neurite networks in a time- and dose-dependent manner. These findings suggest that AMD-induced lysosomal storage accompanied by enhanced oxidative stress and impaired lysosomal degradation in Schwann cells might be a cause of demyelination in the peripheral nervous system.Entities:
Keywords: Schwann cells; demyelination; in vitro; neurotoxicology; peripheral neuropathy
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Year: 2016 PMID: 27152884 DOI: 10.1111/ejn.13268
Source DB: PubMed Journal: Eur J Neurosci ISSN: 0953-816X Impact factor: 3.386