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Novel cell-based assay reveals associations of circulating serum AhR-ligands with metabolic syndrome and mitochondrial dysfunction

Authors
Park, Wook-HaJun, Dae WonKim, Jin TaekJeong, Jae HoonPark, HyokeunChang, Yoon-SeokPark, Kyong SooLee, Hong KyuPak, Youngmi Kim
Issue Date
Jul-2013
Publisher
WILEY
Keywords
dioxins; POPs; aryl hydrocarbon receptor; obesity; metabolic syndrome; insulin resistance; mitochondrial dysfunction; alternative test method development
Citation
BIOFACTORS, v.39, no.4, pp.494 - 504
Indexed
SCIE
SCOPUS
Journal Title
BIOFACTORS
Volume
39
Number
4
Start Page
494
End Page
504
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/162396
DOI
10.1002/biof.1092
ISSN
0951-6433
Abstract
Serum concentrations of environmental pollutants have been positively correlated with diabetes and metabolic syndrome in epidemiologic studies. In turn, abnormal mitochondrial function has been associated with the diseases. The relationships between these variables, however, have not been studied. We developed novel cell-based aryl hydrocarbon receptor (AhR) agonist bioassay system without solvent extraction process and analyzed whether low-dose circulating AhR ligands in human serum are associated with parameters of metabolic syndrome and mitochondrial function. Serum AhR ligand activities were measured as serum 2,3,7,8-tetrachlorodibenzo-p-dioxin equivalent (sTCDDeq) in pM using 10 L human sera from 97 Korean participants (47 with glucose intolerance and 50 matched controls, average age of 46.6 +/- 9.9 years, 53 male and 45 female). sTCDDeq were higher in participants with glucose intolerance than normal controls and were positively associated (P < 0.01) with obesity, blood pressure, serum triglyceride, and fasting glucose, but not with HDL-cholesterol. Body mass index was in a positive linear relationship with serum AhR ligands in healthy participants. When myoblast cells were incubated with human sera, ATP generating power of mitochondria became impaired in an AhR ligand concentration-dependent manner. Our results support that circulating AhR ligands may directly reduce mitochondrial function in tissues, leading to weight gain, glucose intolerance, and metabolic syndrome. Our rapid cell-based assay using minute volume of human serum may provide one of the best monitoring systems for circulating AhR ligands, good clinical biomarkers for the progress of disease and therapeutic efficacy.
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