In vitro profiling of the endocrine-disrupting potency of brominated flame retardants

Timo Hamers, Jorke H. Kamstra, Edwin Sonneveld, Albertinka J. Murk, Monique H.A. Kester, Patrik L. Andersson, Juliette Legler, Abraham Brouwer

    Research output: Contribution to journalArticleAcademicpeer-review

    Abstract

    Over the last few years, increasing evidence has become available that some brominated flame retardants (BFRs) may have endocrine-disrupting (ED) potencies. The goal of the current study was to perform a systematic in vitro screening of the ED potencies of BFRs (1) to elucidate possible modes of action of BFRs in man and wildlife and (2) to classify BFRs with similar profiles of ED potencies. A test set of 27 individual BFRs were selected, consisting of 19 polybrominated diphenyl ether congeners, tetrabromobisphenol-A, hexabromocyclododecane, 2,4,6-tribromophenol, ortho-hydroxylated brominated diphenyl ether 47, and tetrabromobisphenol-A-bis(2,3)dibromopropyl ether. All BFRs were tested for their potency to interact with the arylhydrocarbon receptor, androgen receptor (AR), progesterone receptor (PR), and estrogen receptor. In addition, all BFRs were tested for their potency to inhibit estradiol (sulfation by estradiol sulfotransferase (E2SULT), to interfere with thyroid hormone 3,3′,5-trüodothyronine (T3)-mediated cell proliferation, and to compete with T3-precursor thyroxine for binding to the plasma transport protein transthyretin (TTR). The results of the in vitro screening indicated that BFRs have ED potencies, some of which had not or only marginally been described before (AR antagonism, PR antagonism, E2SULT inhibition, and potentiation of T3-mediated effects). For some BFRs, the potency to induce AR antagonism, E2SULT inhibition, and TTR competition was higher than for natural ligands or clinical drugs used as positive controls. Based on their similarity in ED profiles, BFRs were classified into five different clusters. These findings support further investigation of the potential ED effects of these environmentally relevant BFRs in man and wildlife. © 2006 Oxford University Press.
    Original languageEnglish
    Pages (from-to)157-173
    Number of pages17
    JournalToxicological Sciences
    Volume92
    Issue number1
    DOIs
    Publication statusPublished - 1 Jul 2006

    Keywords

    • Brominated flame retardants
    • Endocrine disruption
    • Hierarchical cluster analysis
    • Principal component analysis
    • Toxicity profiling
    • 2 hydroxylated brominated diphenyl ether 47
    • 2,4,6 tribromophenol
    • 4,4' isopropylidenediphenol
    • androgen receptor
    • aromatic hydrocarbon receptor
    • bromine derivative
    • endocrine disruptor
    • environmental chemical
    • estradiol
    • estrogen receptor
    • flame retardant
    • hexabromocyclododecane
    • ligand
    • liothyronine
    • organohalogen derivative
    • polybrominated diphenyl ether
    • transthyretin
    • progesterone receptor
    • sulfotransferase
    • tetrabromobisphenol A
    • tetrabromobisphenol A bis(2,3)dibromopropyl ether
    • thyroxine
    • unclassified drug
    • animal cell
    • article
    • binding competition
    • cell proliferation
    • chemical interaction
    • controlled study
    • cytotoxicity
    • enzyme inhibition
    • hormone protein complex
    • human
    • human cell
    • in vitro study
    • inhibition kinetics
    • nonhuman
    • protein binding
    • receptor blocking
    • screening
    • sulfation
    • wildlife

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