| Literature DB >> 32283380 |
Chunfeng Xie1, Miaomiao Ge1, Jianliang Jin2, Haie Xu3, Li Mao4, Shanshan Geng1, Jieshu Wu1, Jianyun Zhu5, Xiaoting Li6, Caiyun Zhong7.
Abstract
Bisphenol S is considered as a safer alternative to bisphenol A. In the present study, we used murine macrophages to investigate the effects of BPS exposure on oxidative stress and inflammatory response as well as the underlying mechanism. Cells were exposed to BPS at various concentrations for short period of times. Results showed that 10-8 M BPS triggered oxidative stress by increasing ROS/RNS production, increased the levels of oxidant enzyme NOX1/2, and decreased the levels of antioxidant enzymes SOD1/2, CAT and GSH-Px. 10-8 M BPS exposure significantly induced the production of proinflammatory mediators. Activation of the NLRP3 inflammasome, TLR4, and MAPK pathways was involved in this process. Furthermore, we illustrated that NAC pretreatment diminished these effects triggered by BPS exposure. Collectively, our data suggested that BPS at a dose relevant to human serum concentration induced oxidative stress and inflammatory response in macrophages. These novel findings shed light on the concerns regarding the potential adverse effects of BPS exposure that requires further careful attention.Entities:
Keywords: Bisphenol S; Inflammation; NOD-like receptor protein 3 inflammasome; Oxidative stress; Toll like receptor 4
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Year: 2020 PMID: 32283380 DOI: 10.1016/j.jhazmat.2020.122549
Source DB: PubMed Journal: J Hazard Mater ISSN: 0304-3894 Impact factor: 10.588