论文信息 - A structure–activity relationship linking non-planar PCBs to functional deficits of neural crest cells: new roles for connexins

A structure–activity relationship linking non-planar PCBs to functional deficits of neural crest cells: new roles for connexins

Migration of neural crest cells (NCC) is a fundamental developmental process, and test methods to identify interfering toxicants have been developed. By examining cell function endpoints, as in the ‘migration-inhibition of NCC (cMINC)’ assay, a large number of toxicity mechanisms and protein targets can be covered. However, the key events that lead to the adverse effects of a given chemical or group of related compounds are hard to elucidate. To address this issue, we explored here, whether the establishment of two overlapping structure–activity relationships (SAR)—linking chemical structure on the one hand to a phenotypic test outcome, and on the other hand to a mechanistic endpoint—was useful as strategy to identify relevant toxicity mechanisms. For this purpose, we chose polychlorinated biphenyls (PCB) as a large group of related, but still toxicologically and physicochemically diverse structures. We obtained concentration-dependent data for 26 PCBs in the cMINC assay. Moreover, the test chemicals were evaluated by a new high-content imaging method for their effect on cellular re-distribution of connexin43 and for their capacity to inhibit gap junctions. Non-planar PCBs inhibited NCC migration. The potency (1–10 µM) correlated with the number of ortho-chlorine substituents; non-ortho-chloro (planar) PCBs were non-toxic. The toxicity to NCC partially correlated with gap junction inhibition, while it fully correlated (p < 0.0004) with connexin43 cellular re-distribution. Thus, our double-SAR strategy revealed a mechanistic step tightly linked to NCC toxicity of PCBs. Connexin43 patterns in NCC may be explored as a new endpoint relevant to developmental toxicity screening.

[1] S. Safe,et al. Polychlorinated biphenyls (PCBs): environmental impact, biochemical and toxic responses, and implications for risk assessment. , 1994, Critical reviews in toxicology.

[2] Marcel Leist,et al. Food for thought ... considerations and guidelines for basic test method descriptions in toxicology. , 2010, ALTEX.

[3] Cyrille A M Krul,et al. Development of a panel of high-throughput reporter-gene assays to detect genotoxicity and oxidative stress. , 2014, Mutation research. Genetic toxicology and environmental mutagenesis.

[4] F. Fonnum,et al. Non-dioxin-like PCBs inhibit [(3)H]WIN-35,428 binding to the dopamine transporter: a structure-activity relationship study. , 2013, Neurotoxicology.

[5] S. H. Bennekou,et al. Adverse outcome pathways: opportunities, limitations and open questions , 2017, Archives of Toxicology.

[6] J. Trosko,et al. Inhibition of gap junctional intercellular communication in normal human breast epithelial cells after treatment with pesticides, PCBs, and PBBs, alone or in mixtures. , 1996, Environmental health perspectives.

[7] Marcel Leist,et al. Assessment of chemical-induced impairment of human neurite outgrowth by multiparametric live cell imaging in high-density cultures. , 2011, Toxicological sciences : an official journal of the Society of Toxicology.

[8] C. Lo,et al. Connexin 43 expression in the mouse embryo: Localization of transcripts within developmentally significant domains , 1992, Developmental dynamics : an official publication of the American Association of Anatomists.

[9] Abraham Brouwer,et al. Development of androgen- and estrogen-responsive bioassays, members of a panel of human cell line-based highly selective steroid-responsive bioassays. , 2004, Toxicological sciences : an official journal of the Society of Toxicology.

[10] N. Plant,et al. Non-coplanar polychlorinated biphenyls (PCBs) are direct agonists for the human pregnane-X receptor and constitutive androstane receptor, and activate target gene expression in a tissue-specific manner. , 2012, Toxicology and applied pharmacology.

[11] F. Fonnum,et al. Effect of polychlorinated biphenyls on the uptake of dopamine into rat brain synaptic vesicles: a structure-activity study. , 2001, Toxicology and applied pharmacology.

[12] W. Shain,et al. Neurotoxicity of polychlorinated biphenyls: structure-activity relationship of individual congeners. , 1991, Toxicology and applied pharmacology.

[13] A. A. Jensen. Background levels in humans , 1989 .

[14] Nils Blüthgen,et al. Grouping of histone deacetylase inhibitors and other toxicants disturbing neural crest migration by transcriptional profiling. , 2015, Neurotoxicology.

[15] T. Hamers,et al. In vitro toxicity profiling of ultrapure non-dioxin-like polychlorinated biphenyl congeners and their relative toxic contribution to PCB mixtures in humans. , 2011, Toxicological sciences : an official journal of the Society of Toxicology.

[16] Dorit Merhof,et al. Evaluation of a human neurite growth assay as specific screen for developmental neurotoxicants , 2013, Archives of Toxicology.

[17] M. Kirby,et al. Gap Junction–mediated Cell–Cell Communication Modulates Mouse Neural Crest Migration , 1998, The Journal of cell biology.

[18] O. Boyman,et al. Inflammation-Induced CCR7 Oligomers Form Scaffolds to Integrate Distinct Signaling Pathways for Efficient Cell Migration. , 2016, Immunity.

[19] C. Chaumontet,et al. Altered function, localization and phosphorylation of gap junctions in rat liver epithelial, IAR 20, cells after treatment with PCBs or TCDD. , 1997, Environmental toxicology and pharmacology.

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

[21] Joanne M Yeakley,et al. A trichostatin A expression signature identified by TempO-Seq targeted whole transcriptome profiling , 2017, PloS one.

[22] R. Kaufman,et al. Glycoprotein folding and quality-control mechanisms in protein-folding diseases , 2014, Disease Models & Mechanisms.

[23] K. Kenne,et al. Inhibition of cell-cell communication by methylsulfonyl metabolites of polychlorinated biphenyl congeners in rat liver epithelial IAR 20 cells , 1998, Archives of Toxicology.

[24] K. Willecke,et al. Analysis of connexin expression during mouse Schwann cell development identifies Connexin29 as a novel marker for the transition of neural crest to precursor cells , 2007, Glia.

[25] T. Albertson,et al. Structure-activity relationship for noncoplanar polychlorinated biphenyl congeners toward the ryanodine receptor-Ca2+ channel complex type 1 (RyR1). , 2006, Chemical research in toxicology.

[26] M. Maes,et al. Inhibitors of connexin and pannexin channels as potential therapeutics , 2017, Pharmacology & therapeutics.

[27] Bas J Blaauboer,et al. Dose metric considerations in in vitro assays to improve quantitative in vitro-in vivo dose extrapolations. , 2015, Toxicology.

[28] I. Pessah,et al. Structure-activity relationship of non-coplanar polychlorinated biphenyls toward skeletal muscle ryanodine receptors in rainbow trout (Oncorhynchus mykiss). , 2013, Aquatic toxicology.

[29] A. G. Gittenberger-de Groot,et al. Connexin43 levels are increased in mouse neural crest cells exposed to homocysteine. , 2006, Birth defects research. Part A, Clinical and molecular teratology.

[30] F. Francini,et al. Non-dioxin-like organic toxicant PCB153 modulates sphingolipid metabolism in liver progenitor cells: its role in Cx43-formed gap junction impairment , 2017, Archives of Toxicology.

[31] K. Kenne,et al. The ability to alter the gap junction protein expression outside GST-P positive foci in liver of rats was associated to the tumour promotion potency of different polychlorinated biphenyls. , 1997, Chemico-biological interactions.

[32] R Core Team,et al. R: A language and environment for statistical computing. , 2014 .

[33] D. Laird,et al. Lysosomal and Proteasomal Degradation Play Distinct Roles in the Life Cycle of Cx43 in Gap Junctional Intercellular Communication-deficient and -competent Breast Tumor Cells* , 2003, Journal of Biological Chemistry.

[34] V. Krutovskikh,et al. Alteration in expression of gap junction proteins in rat liver after treatment with the tumour promoter 3,4,5,3',4'-pentachlorobiphenyl. , 1994, Carcinogenesis.

[35] Mardas Daneshian,et al. Reference compounds for alternative test methods to indicate developmental neurotoxicity (DNT) potential of chemicals: example lists and criteria for their selection and use , 2016, ALTEX.

[36] S. Linden,et al. A Panel of Quantitative Calux® Reporter Gene Assays for Reliable High‐Throughput Toxicity Screening of Chemicals and Complex Mixtures , 2013 .

[37] A. Kriegstein,et al. Gap junction adhesion is necessary for radial migration in the neocortex , 2007, Nature.

[38] J. Rahnenführer,et al. Impairment of human neural crest cell migration by prolonged exposure to interferon-beta , 2017, Archives of Toxicology.

[39] Jens C. Streibig,et al. Bioassay analysis using R , 2005 .

[40] J. Gilleron,et al. Accelerated internalization of junctional membrane proteins (connexin 43, N-cadherin and ZO-1) within endocytic vacuoles: an early event of DDT carcinogenicity. , 2008, Biochimica et biophysica acta.

[41] R. Vassena,et al. Exposure of pig oocytes to PCBs during in vitro maturation: effects on developmental competence, cytoplasmic remodelling and communications with cumulus cells. , 2004, European journal of histochemistry : EJH.

[42] D. Laird,et al. Gap junction turnover, intracellular trafficking, and phosphorylation of connexin43 in brefeldin A-treated rat mammary tumor cells , 1995, The Journal of cell biology.

[43] I. Choi,et al. Tissue-based metabolic labeling of polysialic acids in living primary hippocampal neurons , 2015, Proceedings of the National Academy of Sciences.

[44] J. Lodge. Air quality guidelines for Europe: WHO regional publications, European series, No. 23, World Health Organization, 1211 Geneva 27, Switzerland; WHO publications center USA, 49 Sheridan Avenue, Albany, NY 12210, 1987, xiii + 426 pp. price: Sw. fr. 60 , 1988 .

[45] Emiel Rorije,et al. A high throughput screening system for predicting chemically-induced reproductive organ deformities. , 2015, Reproductive toxicology.

[46] Philippe Soriano,et al. Inhibition of Gap Junction Communication at Ectopic Eph/ephrin Boundaries Underlies Craniofrontonasal Syndrome , 2006, PLoS biology.

[47] P. Kodavanti. Neurotoxicity of Persistent Organic Pollutants: Possible Mode(S) of Action and Further Considerations , 2005, Dose-response : a publication of International Hormesis Society.

[48] R. Westerink,et al. Modulation of cell viability, oxidative stress, calcium homeostasis, and voltage- and ligand-gated ion channels as common mechanisms of action of (mixtures of) non-dioxin-like polychlorinated biphenyls and polybrominated diphenyl ethers , 2013, Environmental Science and Pollution Research.

[49] K. Schalper,et al. Possible role of hemichannels in cancer , 2014, Front. Physiol..

[50] D. Laird. Connexin phosphorylation as a regulatory event linked to gap junction internalization and degradation. , 2005, Biochimica et biophysica acta.

[51] J. Trosko,et al. Changes in gap‐junction permeability, phosphorylation, and number mediated by phorbol ester and non‐phorbol‐ester tumor promoters in rat liver epithelial cells , 1994, Molecular carcinogenesis.

[52] P. Carlen,et al. Changes in Neuronal Migration in Neocortex of Connexin43 Null Mutant Mice , 2003, Journal of neuropathology and experimental neurology.

[53] Wolfgang Huber,et al. EBImage—an R package for image processing with applications to cellular phenotypes , 2010, Bioinform..

[54] A. Kozubík,et al. The 2,2',4,4',5,5'-hexachlorobiphenyl-enhanced degradation of connexin 43 involves both proteasomal and lysosomal activities. , 2009, Toxicological sciences : an official journal of the Society of Toxicology.

[55] P. Kameritsch,et al. The carboxyl tail of Cx43 augments p38 mediated cell migration in a gap junction-independent manner. , 2010, European journal of cell biology.

[56] J. G. Hengstler,et al. Profiling of drugs and environmental chemicals for functional impairment of neural crest migration in a novel stem cell-based test battery , 2014, Archives of Toxicology.

[57] Yihe Guo,et al. Gap junction-microtubule associations in rat alveolar epithelial cells. , 2003, American journal of physiology. Lung cellular and molecular physiology.

[58] M. DeVito,et al. NON-DIOXIN-LIKE PCBs: EFFECTS AND CONSIDERATION IN ECOLOGICAL RISK ASSESSMENT by , 2003 .

[59] J. Jacobson,et al. Effects of exposure to PCBs and related compounds on growth and activity in children. , 1990, Neurotoxicology and teratology.

[60] Jian Du,et al. Metabolic glycoengineering: sialic acid and beyond. , 2009, Glycobiology.

[61] A. E. Wiencken-barger,et al. A role for Connexin43 during neurodevelopment , 2007, Glia.

[62] B. Giepmans,et al. The gap junction protein connexin43 interacts with the second PDZ domain of the zona occludens-1 protein , 1998, Current Biology.

[63] W. Reutter,et al. Two-color glycan labeling of live cells by a combination of Diels-Alder and click chemistry. , 2013, Angewandte Chemie.

[64] R. Gourdie,et al. Zonula occludens-1 alters connexin43 gap junction size and organization by influencing channel accretion. , 2005, Molecular biology of the cell.

[65] Heiko Lemcke,et al. Neuronal differentiation requires a biphasic modulation of gap junctional intercellular communication caused by dynamic changes of connexin43 expression , 2013, The European journal of neuroscience.

[66] Yong Woo Lee,et al. PCB 104-induced proinflammatory reactions in human vascular endothelial cells: relationship to cancer metastasis and atherogenesis. , 2003, Toxicological sciences : an official journal of the Society of Toxicology.

[67] Tanja Waldmann,et al. Design of a high-throughput human neural crest cell migration assay to indicate potential developmental toxicants. , 2016, ALTEX.

[68] C. Naus,et al. The carboxy‐terminal tail of connexin43 gap junction protein is sufficient to mediate cytoskeleton changes in human glioma cells , 2010, Journal of cellular biochemistry.

[69] Alice Krebs,et al. Combination of multiple neural crest migration assays to identify environmental toxicants from a proof-of-concept chemical library , 2017, Archives of Toxicology.

[70] Marcel Leist,et al. Evaluation of Developmental Toxicants and Signaling Pathways in a Functional Test Based on the Migration of Human Neural Crest Cells , 2012, Environmental health perspectives.

[71] C. Naus,et al. Connexin43 enhances glioma invasion by a mechanism involving the carboxy terminus , 2007, Glia.

[72] J. Jacobson,et al. Intellectual impairment in children exposed to polychlorinated biphenyls in utero. , 1996, The New England journal of medicine.

[73] R. Francis,et al. Connexin 43 regulates epicardial cell polarity and migration in coronary vascular development , 2009, Development.

[74] D. Laird,et al. The tumor-suppressive function of Connexin43 in keratinocytes is mediated in part via interaction with caveolin-1. , 2010, Cancer research.

[75] M. E. Hahn,et al. Relative contributions of affinity and intrinsic efficacy to aryl hydrocarbon receptor ligand potency. , 2000, Toxicology and applied pharmacology.

[76] R. Ruch,et al. Gap junction endocytosis and lysosomal degradation of connexin43-P2 in WB-F344 rat liver epithelial cells treated with DDT and lindane. , 1996, Carcinogenesis.

[77] J. Trosko,et al. Inhibition of gap junctional intercellular communication by noncoplanar polychlorinated biphenyls: inhibitory potencies and screening for potential mode(s) of action. , 2003, Toxicological sciences : an official journal of the Society of Toxicology.

[78] Jennifer A. Prescher,et al. Chemistry in living systems , 2005, Nature chemical biology.

[79] H. J. Miller,et al. WORLD PCBs MAP: STORAGE AND EFFECTS IN MAN AND HIS BIOLOGIC ENVIRONMENT IN THE 1970s , 1979, Annals of the New York Academy of Sciences.

[80] J. Giesy,et al. Species-specific recombinant cell lines as bioassay systems for the detection of 2,3,7,8-tetrachlorodibenzo-p-dioxin-like chemicals. , 1996, Fundamental and applied toxicology : official journal of the Society of Toxicology.

[81] T. Steinberg,et al. Connexin43 Deficiency Causes Delayed Ossification, Craniofacial Abnormalities, and Osteoblast Dysfunction , 2000, The Journal of cell biology.

[82] T. Brümmendorf,et al. Accelerated telomere shortening in peripheral blood lymphocytes after occupational polychlorinated biphenyls exposure , 2016, Archives of Toxicology.

[83] R. Denver,et al. Mechanisms and significance of nuclear receptor auto- and cross-regulation. , 2011, General and comparative endocrinology.

[84] Yang Luo,et al. Modulation of mouse neural crest cell motility by N-cadherin and connexin 43 gap junctions , 2001, The Journal of cell biology.

[85] R. Francis,et al. Connexin 43-mediated modulation of polarized cell movement and the directional migration of cardiac neural crest cells , 2006, Development.

[86] D. Legler,et al. Common and biased signaling pathways of the chemokine receptor CCR7 elicited by its ligands CCL19 and CCL21 in leukocytes , 2016, Journal of leukocyte biology.

[87] Mardas Daneshian,et al. Highlight report: Launch of a large integrated European in vitro toxicology project: EU-ToxRisk , 2016, Archives of Toxicology.

[88] C. Naus,et al. Involvement of the Cytoplasmic C-Terminal Domain of Connexin43 in Neuronal Migration , 2009, The Journal of Neuroscience.

[89] P. Arvan,et al. Secretory Pathway Quality Control Operating in Golgi, Plasmalemmal, and Endosomal Systems , 2002, Traffic.

[90] B. Chatterjee,et al. Connexin43 Modulates Cell Polarity and Directional Cell Migration by Regulating Microtubule Dynamics , 2011, PloS one.

[91] U. Ahlborg,et al. Inhibition of dye transfer in rat liver WB cell culture by polychlorinated biphenyls. , 1991, Pharmacology & toxicology.