Interaction between Bisphenol Derivatives and Protein Disulphide Isomerase (PDI) and Inhibition of PDI Functions: Requirement of Chemical Structure for Binding to PDI

doi:10.1093/jb/mvn075

Journal of Biochemistry Advance Access originally published online on May 31, 2008
Journal of Biochemistry 2008 144(3):335-342; doi:10.1093/jb/mvn075

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Interaction between Bisphenol Derivatives and Protein Disulphide Isomerase (PDI) and Inhibition of PDI Functions: Requirement of Chemical Structure for Binding to PDI

Shoko Hashimoto, Kazushi Okada^* and Susumu Imaoka

Department of Bioscience, Nanobiotechnology Research Center, School of Science and Technology, Kwansei Gakuin University, 2-1 Gakuen, Sanda 669-1337, Japan

*To whom correspondence should be addressed. Tel/Fax: +81-79-565-7673, E-mail: bhp46831{at}kwansei.ac.jp

Received April 11, 2008; Accepted May 19, 2008

Abstract

Bisphenol A (BPA) is an endocrine disrupting chemical and severalbiological effects have been reported. Previously, protein disulphideisomerase (PDI) was isolated as a target molecule of bisphenolA. In this study, to clarify the effects of BPA on PDI functions,we investigated the relationship between the chemical structureof BPA derivatives and the effects on PDI-mediated isomeraseand chaperone activity. We also investigated the effects ofchanges in the isomerase domain of PDI on the binding of chemicals,using PDI mutants and oxidized or reduced PDI. Among six chemicals,only chemicals, which have a phenol group, can bind to PDI andthese chemicals also have an inhibitory effect on PDI-mediatedisomerase activity. Changes in the structure of the PDI isomerasedomain did not affect chemical-binding activity. On the otherhand, the chemicals used in this study have low effects on chaperoneactivity of PDI. Substitutions in Cys residues (Cys398 and Cys401)of the isomerase active site changed chaperone activity. Thepresent study indicates that phenolic compounds specificallybind to PDI and inhibit isomerase activity. This study providesuseful information to predict the biological effects of chemicalsand structural studies of PDI containing the function of chemicalbinding.

Key Words: bisphenol A, protein disulphide isomerase (PDI), dimethyl bisphenol A, chaperone activity, protein folding

Abbreviations: ADH, alcohol dehydrogenase; BPA, Bisphenol A, 2,2-bis(4-hydroxyphenyl)-propane; BPE, Bisphenol E, 1,1-bis(4-hydroxyphenyl)ethane; BPF, Bisphenol F, 4,4-methylenebisphenol; Cumylphenol, 4- ${alpha}$ -Cumylphenol; DMBPA, dimethylbisphenol A, 2,2-bis(4-methoxyphenyl)propane; HIF-1 ${alpha}$ , hypoxia-inducible factor-1 ${alpha}$ ; mBBr, monobromobimane; PDI, protein disulphide isomerase; RNase A, ribonuclease A; T3, 3,3',5-triiodo-L-thyronine

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