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Antioxidant and Neuroprotective Effects of Paeonol against Oxidative Stress and Altered Carrier-Mediated Transport System on NSC-34 Cell Linesopen access

Authors
Latif, SanaChoi, Seung-HyeGyawali, AsmitaHyeon, Seung JaeKang, Young-SookRyu, Hoon
Issue Date
Jul-2022
Publisher
MDPI
Keywords
paeonol; neuroprotection; reduction-oxidation reactions; carrier-mediated transport system; organic anion transporter 1 (Oat1); plasma membrane monoamine transporter (Pmat); amyotrophic lateral sclerosis (ALS); NSC-34 cell lines
Citation
ANTIOXIDANTS, v.11, no.7
Journal Title
ANTIOXIDANTS
Volume
11
Number
7
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/152620
DOI
10.3390/antiox11071392
ISSN
2076-3921
2076-3921
Abstract
Paeonol is a naturally occurring phenolic agent that attenuates neurotoxicity in neurodegenerative diseases. We aimed to investigate the antioxidant and protective effects of paeonol and determine its transport mechanism in wild-type (WT; NSC-34/hSOD1(WT)) and mutant-type (MT; NSC-34/hSOD1(G93A)) motor neuron-like amyotrophic lateral sclerosis (ALS) cell lines. Cytotoxicity induced by glutamate, lipopolysaccharides, and H2O2 reduced viability of cell; however, the addition of paeonol improved cell viability against neurotoxicity. The [H-3]paeonol uptake was increased in the presence of H2O2 in both cell lines. Paeonol recovered ALS model cell lines by reducing mitochondrial oxidative stress induced by glutamate. The transport of paeonol was time-, concentration-, and pH-dependent in both NSC-34 cell lines. Kinetic parameters showed two transport sites with altered affinity and capacity in the MT cell line compared to the WT cell line. [H-3]Paeonol uptake increased in the MT cell line transfected with organic anion transporter1 (Oat1)/Slc22a6 small interfering RNA compared to that in the control. Plasma membrane monoamine transporter (Pmat) was also involved in the uptake of paeonol by ALS model cell lines. Overall, paeonol exhibits neuroprotective activity via a carrier-mediated transport system and may be a beneficial therapy for preventing motor neuronal damage under ALS-like conditions.
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