4.7 Article

The environmental endocrine disruptor p-nitrophenol interacts with FKBP51, a positive regulator of androgen receptor and inhibits androgen receptor signaling in human cells

期刊

JOURNAL OF HAZARDOUS MATERIALS
卷 307, 期 -, 页码 193-201

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.jhazmat.2015.12.045

关键词

p-Nitrophenol; FKBP51; Androgen receptor; Molecular dynamics simulation; Crystal structure

资金

  1. National Natural Science Foundation of China [31300616, 81172437]
  2. Fundamental Research Funds for the Central Universities from Lanzhou University [lzujbky-2014-85, lzujbky-2015-k18]

向作者/读者索取更多资源

The compound p-nitrophenol, which shows the anti-androgenic activity, can easily become anthropogenic pollutants and pose a threat to the environment and human health. Previous work indicates that the anti-androgenic mechanism of p-nitrophenol is complex and may involve several components in the AR signaling pathway, but the molecular details of how p-nitrophenol inhibits AR signaling are still not quite clear. Here, we characterized p-nitrophenol binds to the FK1 domain of an AR positive regulator FKBP51 with micromolar affinity and structural analysis of FK1 domain in complex with p-nitrophenol revealed that p-nitrophenol occupies a hydrophobic FK1 pocket that is vital for AR activity enhancement. Molecular dynamics simulation indicated that p-nitrophenol is stably bound to the FK1 pocket and the hotspot residues that involved p-nitrophenol binding are mainly hydrophobic and overlap with the AR interaction site. Furthermore, we showed that p-nitrophenol inhibits the androgen-dependent growth of human prostate cancer cells, possibly through down-regulating the expression levels of AR activated downstream genes. Taken together, our data suggests that p-nitrophenol suppresses the AR signaling pathway at least in part by blocking the interaction between AR and its positive regulator FKBP51. We believe that our findings could provide new guidelines for assessing the potential health effects of p-nitrophenol. (C) 2015 Elsevier B.V. All rights reserved.

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