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Toxicology. 2018 Jan 15;393:171-184. doi: 10.1016/j.tox.2017.11.004. Epub 2017 Nov 8.

Cytoprotection of lipoic acid against toxicity induced by saxitoxin in hippocampal cell line HT-22 through in silico modeling and in vitro assays.

Author information

1
Institute of Biological Science, Federal University of Rio Grande - FURG, Rio Grande, RS, Brazil; Post-Graduate Program in Physiological Sciences - Rio Grande, RS, Brazil. Electronic address: pattybramos@gmail.com.
2
Cyanobacteria and Ficotoxin Laboratory, FURG, Rio Grande, RS, Brazil.
3
Institute of Biological Science, Federal University of Rio Grande - FURG, Rio Grande, RS, Brazil.
4
Institute of Biological Science, Federal University of Rio Grande - FURG, Rio Grande, RS, Brazil; Post-Graduate Program in Physiological Sciences - Rio Grande, RS, Brazil.
5
Center of Computational Science (C3), FURG, Rio Grande, RS, Brazil.
6
Franciscan University Center, UNIFRA, Santa Maria, RS, Brazil; Post-Graduate Program in Nanoscience, UNIFRA, Santa Maria, RS, Brazil.

Abstract

Saxitoxins (STXs) are potent neurotoxins that block voltage-gated channels in neurons and induce cytotoxicity. These toxins not only can generate reactive oxygen species but also can alter antioxidant levels, promoting oxidative stress. Under this pro-oxidant situation, the use of the antioxidant lipoic acid (LA) can represent a chemoprotective alternative to minimize the deleterious effects induced by neurotoxins as STXs. P-glycoprotein (P-gp) is a well-known ATP-binding cassette (ABC) transporter that plays a crucial role in the extrusion of toxic substances, decreasing their accumulation and potential intracellular effects in virtue of its broad substrate specificity, its expression in many excretory tissues and its large efflux capacity. The interaction of STXs with LA was evaluated by ab initio simulation, molecular docking and bioassays using the cell line HT-22. The interaction of STXs with LA occurs by physisorption. Molecular docking indicated that STXs can be a substrate of P-gp and, estimating the Free Energy of Binding (FEB), LA has lower amino acids residues binding sites, similar to verapamil, while STX and STX+LA_1 have similar amino acids residues and binding sites with similar FEB between this ligands.Cells were exposed to STXs and LA for 30min and 24h. LA treatment minimizes STX cytotoxicity, evaluated by trypan blue and MTT assay and both STX and STX-LA treatments were efficient to induce P-gp activity measured by rhodamine 123 dye extrusion. LA and STX+LA treatments induced low reactive oxygen species levels and low oxygen consumption. Based on our results, it can be concluded that LA was able to induce cytoprotection, including induction of cellular glutathione levels, and that STX+LA interaction reduced toxicity effects induced by STX. Overall, the in vitro results corroborated the semi-empirical evidences found using density functional theory ab initio simulation and molecular docking.

KEYWORDS:

Antioxidant; Molecular docking; Neurotoxin; P-glycoprotein

PMID:
29128272
DOI:
10.1016/j.tox.2017.11.004
[Indexed for MEDLINE]

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