论文信息 - Thyroid-Hormone–Disrupting Chemicals: Evidence for Dose-Dependent Additivity or Synergism

Thyroid-Hormone–Disrupting Chemicals: Evidence for Dose-Dependent Additivity or Synergism

Endocrine disruption from environmental contaminants has been linked to a broad spectrum of adverse outcomes. One concern about endocrine-disrupting xenobiotics is the potential for additive or synergistic (i.e., greater-than-additive) effects of mixtures. A short-term dosing model to examine the effects of environmental mixtures on thyroid homeostasis has been developed. Prototypic thyroid-disrupting chemicals (TDCs) such as dioxins, polychlorinated biphenyls (PCBs), and poly-brominated diphenyl ethers have been shown to alter thyroid hormone homeostasis in this model primarily by up-regulating hepatic catabolism of thyroid hormones via at least two mechanisms. Our present effort tested the hypothesis that a mixture of TDCs will affect serum total thyroxine (T4) concentrations in a dose-additive manner. Young female Long-Evans rats were dosed via gavage with 18 different polyyhalogenated aromatic hydrocarbons [2 dioxins, 4 dibenzofurans, and 12 PCBs, including dioxin-like and non-dioxin-like PCBs] for 4 consecutive days. Serum total T4 was measured via radioimmunoassay in samples collected 24 hr after the last dose. Extensive dose–response functions (based on seven to nine doses per chemical) were determined for individual chemicals. A mixture was custom synthesized with the ratio of chemicals based on environmental concentrations. Serial dilutions of this mixture ranged from approximately background levels to 100-fold greater than background human daily intakes. Six serial dilutions of the mixture were tested in the same 4-day assay. Doses of individual chemicals that were associated with a 30% TH decrease from control (ED30), as well as predicted mixture outcomes were calculated using a flexible single-chemical-required method applicable to chemicals with differing dose thresholds and maximum-effect asymptotes. The single-chemical data were modeled without and with the mixture data to determine, respectively, the expected mixture response (the additivity model) and the experimentally observed mixture response (the empirical model). A likelihood-ratio test revealed statistically significant departure from dose additivity. There was no deviation from additivity at the lowest doses of the mixture, but there was a greater-than-additive effect at the three highest mixtures doses. At high doses the additivity model underpredicted the empirical effects by 2- to 3-fold. These are the first results to suggest dose-dependent additivity and synergism in TDCs that may act via different mechanisms in a complex mixture. The results imply that cumulative risk approaches be considered when assessing the risk of exposure to chemical mixtures that contain TDCs.

[1] S. Loewe. The problem of synergism and antagonism of combined drugs. , 1953, Arzneimittel-Forschung.

[2] M. Surks,et al. Increased thyroxine turnover and thyroidal function after stimulation of hepatocellular binding of thyroxine by phenobarbital. , 1968, The Journal of clinical investigation.

[3] M. Berenbaum. The expected effect of a combination of agents: the general solution. , 1985, Journal of theoretical biology.

[4] P. Hurley. Mode of carcinogenic action of pesticides inducing thyroid follicular cell tumors in rodents. , 1998, British Journal of Cancer.

[5] L. Birnbaum,et al. Disposition of octachlorodibenzo-p-dioxin (OCDD) in male rats. , 1988, Toxicology and applied pharmacology.

[6] P. McCullagh,et al. Generalized Linear Models , 1992 .

[7] A. Levin,et al. The effect of phenobarbital on the metabolism and excretion of thyroxine in rats. , 1989, Toxicology and applied pharmacology.

[8] P. McCullagh,et al. Generalized Linear Models, 2nd Edn. , 1990 .

[9] T. Visser,et al. Multiple UDP‐glucuronyltransferases for the glucuronidation of thyroid hormone with preference for 3,3',5'‐triiodothyronine (reverse T3) , 1993, FEBS letters.

[10] T. Visser,et al. Interference of polychlorinated biphenyls in hepatic and brain thyroid hormone metabolism in fetal and neonatal rats. , 1993, Toxicology and applied pharmacology.

[11] John A. Nelder,et al. Generalized linear models. 2nd ed. , 1993 .

[12] S. Bursian,et al. Contaminants in fishes from Great Lakes-influenced sections and above dams of three Michigan rivers. I: Concentrations of organo chlorine insecticides, polychlorinated biphenyls, dioxin equivalents, and mercury , 1994, Archives of environmental contamination and toxicology.

[13] T. Nilsson,et al. Toxic PCB congeners and organochlorine pesticides in Italian human milk. , 1994, Ecotoxicology and environmental safety.

[14] A. Schecter,et al. Congener-specific levels of dioxins and dibenzofurans in U.S. food and estimated daily dioxin toxic equivalent intake. , 1994, Environmental health perspectives.

[15] L. Needham,et al. Levels of non-ortho-substituted (coplanar), mono- and di-ortho-substituted polychlorinated biphenyls, dibenzo-p-dioxins, and dibenzofurans in human serum and adipose tissue. , 1994, Environmental health perspectives.

[16] A. Schecter,et al. Polychlorinated biphenyl levels in the tissues of exposed and nonexposed humans. , 1994, Environmental health perspectives.

[17] M. van den Berg,et al. The toxicokinetics and metabolism of polychlorinated dibenzo-p-dioxins (PCDDs) and dibenzofurans (PCDFs) and their relevance for toxicity. , 1994, Critical reviews in toxicology.

[18] R. Mcclain. Mechanistic considerations for the relevance of animal data on thyroid neoplasia to human risk assessment. , 1995, Mutation research.

[19] S. Safe,et al. Structure-dependent induction of CYP2B by polychlorinated biphenyl congeners in female Sprague-Dawley rats. , 1995, Biochemical pharmacology.

[20] M. DeVito,et al. Comparisons of estimated human body burdens of dioxinlike chemicals and TCDD body burdens in experimentally exposed animals. , 1995, Environmental health perspectives.

[21] C. Capen,et al. Mechanistic Data and Risk Assessment of Selected Toxic End Points of the Thyroid Gland , 1997, Toxicologic pathology.

[22] L. Hansen,et al. Morphometric changes in the prepubertal female rat thyroid gland following acute exposure to 2,2',4,4'-tetrachlorobiphenyl and Aroclor 1242. , 1997, Journal of toxicology and environmental health.

[23] T. Visser,et al. Interactions of Persistent Environmental Organohalogens With the Thyroid Hormone System: Mechanisms and Possible Consequences for Animal and Human Health , 1998, Toxicology and industrial health.

[24] M. DeVito,et al. Dose-response relationships for disposition and hepatic sequestration of polyhalogenated dibenzo-p-dioxins, dibenzofurans, and biphenyls following subchronic treatment in mice. , 1998, Toxicological sciences : an official journal of the Society of Toxicology.

[25] C. Capen. Correlation of mechanistic data and histopathology in the evaluation of selected toxic endpoints of the endocrine system. , 1998, Toxicology letters.

[26] J. Wolffa. Perchlorate and the Thyroid Gland , 1998 .

[27] T. Crisp,et al. Risk assessment of thyroid follicular cell tumors. , 1998, Environmental health perspectives.

[28] Dose-response relationships for disposition and hepatic sequestration of polyhalogenated dibenzo-p-dioxins, dibenzofurans, and biphenyls following subchronic treatment in mice. , 1998, Toxicological sciences : an official journal of the Society of Toxicology.

[29] Safe,et al. Toxic equivalency factors (TEFs) for PCBs, PCDDs, PCDFs for humans and wildlife. , 1998, Environmental health perspectives.

[30] Cody L. Wilson,et al. Mechanisms of Ligand-Induced Aryl Hydrocarbon Receptor-Mediated Biochemical and Toxic Responses , 1998, Toxicologic pathology.

[31] K. Crofton,et al. Screening methods for thyroid hormone disruptors. , 1999, Environmental health perspectives.

[32] M. Obregon,et al. Is neuropsychological development related to maternal hypothyroidism or to maternal hypothyroxinemia? , 2000, The Journal of clinical endocrinology and metabolism.

[33] P. Furst,et al. Exposure of populations to dioxins and related compounds , 2000, Food additives and contaminants.

[34] C. Klaassen,et al. Effects of microsomal enzyme inducers on outer-ring deiodinase activity toward thyroid hormones in various rat tissues. , 2000, Toxicology and applied pharmacology.

[35] C. Klaassen,et al. Differential effects of microsomal enzyme inducers on in vitro thyroxine (T(4)) and triiodothyronine (T(3)) glucuronidation. , 2000, Toxicological sciences : an official journal of the Society of Toxicology.

[36] K. Crofton,et al. Comparative responsiveness of hypothyroxinemia and hepatic enzyme induction in Long-Evans rats versus C57BL/6J mice exposed to TCDD-like and phenobarbital-like polychlorinated biphenyl congeners. , 2002, Toxicological sciences : an official journal of the Society of Toxicology.

[37] Eric R. Ziegel,et al. Generalized Linear Models , 2002, Technometrics.

[38] C. Klaassen,et al. Increase in rat liver UDP-glucuronosyltransferase mRNA by microsomal enzyme inducers that enhance thyroid hormone glucuronidation. , 2002, Drug metabolism and disposition: the biological fate of chemicals.

[39] M. Lorber. A pharmacokinetic model for estimating exposure of Americans to dioxin-like compounds in the past, present, and future. , 2002, The Science of the total environment.

[40] Rory Conolly,et al. Support of science-based decisions concerning the evaluation of the toxicology of mixtures: a new beginning. , 2002, Regulatory toxicology and pharmacology : RTP.

[41] M. Wade,et al. Thyroid toxicity due to subchronic exposure to a complex mixture of 16 organochlorines, lead, and cadmium. , 2002, Toxicological sciences : an official journal of the Society of Toxicology.

[42] J. Haddow,et al. Thyroid-stimulating-hormone concentrations and risk of hypothyroidism , 2002, The Lancet.

[43] Chris Gennings,et al. Statistical analysis of interactive cytotoxicity in human epidermal keratinocytes following exposure to a mixture of four metals , 2002 .

[44] Terri Damstra,et al. Global assessment of the state-of-the-science of endocrine disruptors , 2002 .

[45] S. Choudhuri,et al. Induction profile of rat organic anion transporting polypeptide 2 (oatp2) by prototypical drug-metabolizing enzyme inducers that activate gene expression through ligand-activated transcription factor pathways. , 2002, The Journal of pharmacology and experimental therapeutics.

[46] M. Khan,et al. The hypothalamo-pituitary-thyroid (HPT) axis: a target of nonpersistent ortho-substituted PCB congeners. , 2002, Toxicological sciences : an official journal of the Society of Toxicology.

[47] J. Groten,et al. Toxicological evaluation of chemical mixtures. , 2002, Food and chemical toxicology : an international journal published for the British Industrial Biological Research Association.

[48] M. Khan,et al. Ortho-substituted polychlorinated biphenyl (PCB) congeners (95 or 101) decrease pituitary response to thyrotropin releasing hormone. , 2003, Toxicology letters.

[49] Robert J Kavlock,et al. Uncertainties for endocrine disrupters: our view on progress. , 2003, Toxicological sciences : an official journal of the Society of Toxicology.

[50] L. Marro,et al. Effects of postnatal exposure to mixtures of non-ortho-PCBs, PCDDs, and PCDFs in prepubertal female rats. , 2003, Toxicological sciences : an official journal of the Society of Toxicology.

[51] Philippe Grandjean,et al. Comparison of polychlorinated biphenyl levels across studies of human neurodevelopment. , 2003, Environmental health perspectives.

[52] K. Crofton. Developmental Disruption of Thyroid Hormone: Correlations with Hearing Dysfunction in Rats , 2004, Risk analysis : an official publication of the Society for Risk Analysis.

[53] J. Ashby,et al. Sensitivity of the immature rat uterotrophic assay to mixtures of estrogens. , 2004, Environmental health perspectives.

[54] Evaluating the Toxicity of Chemical Mixtures , 2004, Environmental health perspectives.

[55] F. Grün,et al. Highly chlorinated PCBs inhibit the human xenobiotic response mediated by the steroid and xenobiotic receptor (SXR). , 2003, Environmental health perspectives.

[56] W. H. Carter,et al. Detecting interaction(s) and assessing the impact of component subsets in a chemical mixture using fixed-ratio mixture ray designs , 2004 .

[57] C. Gennings,et al. A novel flexible approach for evaluating fixed ratio mixtures of full and partial agonists. , 2004, Toxicological sciences : an official journal of the Society of Toxicology.

[58] W. Notten,et al. Interactions of halogenated industrial chemicals with transthyretin and effects on thyroid hormone levels in vivo , 2005, Archives of Toxicology.