Literature DB >> 27116683

Developmental exposure to acetaminophen does not induce hyperactivity in zebrafish larvae.

Isabel Reuter1,2, Sabine Knaup3, Marcel Romanos4, Klaus-Peter Lesch2, Carsten Drepper5, Christina Lillesaar6.   

Abstract

First line pain relief medication during pregnancy relies nearly entirely on the over-the-counter analgesic acetaminophen, which is generally considered safe to use during gestation. However, recent epidemiological studies suggest a risk of developing attention-deficit/hyperactivity disorder (ADHD)-like symptoms in children if mothers use acetaminophen during pregnancy. Currently, there are no experimental proofs that prenatal acetaminophen exposure causes developmental brain alterations of progeny. Exposure to high acetaminophen concentrations causes liver toxicity, which is well investigated in different model organisms. However, sub-liver-toxic concentrations have not been experimentally investigated with respect to ADHD endophenotypes such as hyperactivity. We used zebrafish to investigate the potential impact of acetaminophen exposure on locomotor activity levels, and compared it to the established zebrafish Latrophilin 3 (Lphn3) ADHD-model. We determined the sub-liver-toxic concentration of acetaminophen in zebrafish larvae and treated wild-type and lphn3.1 knockdown larvae with increasing concentrations of acetaminophen. We were able to confirm that lphn3.1 knockdown alone causes hyperactivity, strengthening the implication of Lphn3 dysfunction as an ADHD risk factor. Neither acute nor chronic exposure to acetaminophen at sub-liver-toxic concentrations in wild-type or lphn3.1 knock-downs increases locomotor activity levels. Together our findings show that embryonic to larval exposure to acetaminophen does not cause hyperactivity in zebrafish larvae. Furthermore, there are no additive and/or synergistic effects of acetaminophen exposure in a susceptible background induced by knock-down of lphn3.1. Our experimental study suggests that there is, at least in zebrafish larvae, no direct link between embryonic acetaminophen exposure and hyperactivity. Further work is necessary to clarify this issue in humans.

Entities:  

Keywords:  Acetaminophen; Behavior; Impulsivity; Locomotion; latrophilin3.1

Mesh:

Substances:

Year:  2016        PMID: 27116683     DOI: 10.1007/s00702-016-1556-z

Source DB:  PubMed          Journal:  J Neural Transm (Vienna)        ISSN: 0300-9564            Impact factor:   3.575


  23 in total

1.  High-resolution in situ hybridization to whole-mount zebrafish embryos.

Authors:  Christine Thisse; Bernard Thisse
Journal:  Nat Protoc       Date:  2008       Impact factor: 13.491

2.  Gene expression markers in the zebrafish embryo reflect a hepatotoxic response in animal models and humans.

Authors:  Marja Driessen; Anne S Kienhuis; Alexa P Vitins; Jeroen L A Pennings; Tessa E Pronk; Evert-Jan van den Brandhof; Marianne Roodbergen; Bob van de Water; Leo T M van der Ven
Journal:  Toxicol Lett       Date:  2014-07-24       Impact factor: 4.372

3.  Acetaminophen use during pregnancy, behavioral problems, and hyperkinetic disorders.

Authors:  Zeyan Liew; Beate Ritz; Cristina Rebordosa; Pei-Chen Lee; Jørn Olsen
Journal:  JAMA Pediatr       Date:  2014-04       Impact factor: 16.193

4.  The ADHD-susceptibility gene lphn3.1 modulates dopaminergic neuron formation and locomotor activity during zebrafish development.

Authors:  M Lange; W Norton; M Coolen; M Chaminade; S Merker; F Proft; A Schmitt; P Vernier; K-P Lesch; L Bally-Cuif
Journal:  Mol Psychiatry       Date:  2012-04-17       Impact factor: 15.992

5.  A common variant of the latrophilin 3 gene, LPHN3, confers susceptibility to ADHD and predicts effectiveness of stimulant medication.

Authors:  M Arcos-Burgos; M Jain; M T Acosta; S Shively; H Stanescu; D Wallis; S Domené; J I Vélez; J D Karkera; J Balog; K Berg; R Kleta; W A Gahl; E Roessler; R Long; J Lie; D Pineda; A C Londoño; J D Palacio; A Arbelaez; F Lopera; J Elia; H Hakonarson; S Johansson; P M Knappskog; J Haavik; M Ribases; B Cormand; M Bayes; M Casas; J A Ramos-Quiroga; A Hervas; B S Maher; S V Faraone; C Seitz; C M Freitag; H Palmason; J Meyer; M Romanos; S Walitza; U Hemminger; A Warnke; J Romanos; T Renner; C Jacob; K-P Lesch; J Swanson; A Vortmeyer; J E Bailey-Wilson; F X Castellanos; M Muenke
Journal:  Mol Psychiatry       Date:  2010-02-16       Impact factor: 15.992

6.  A zebrafish phenotypic assay for assessing drug-induced hepatotoxicity.

Authors:  Jian-Hui He; Sheng-Ya Guo; Feng Zhu; Jun-Jing Zhu; Yun-Xiang Chen; Chang-Jiang Huang; Ji-Min Gao; Qiao-Xiang Dong; Yao-Xian Xuan; Chun-Qi Li
Journal:  J Pharmacol Toxicol Methods       Date:  2012-11-03       Impact factor: 1.950

7.  Initial characterization of mice null for Lphn3, a gene implicated in ADHD and addiction.

Authors:  Deeann Wallis; Denise S Hill; Ian A Mendez; Louise C Abbott; Richard H Finnell; Paul J Wellman; Barry Setlow
Journal:  Brain Res       Date:  2012-05-07       Impact factor: 3.252

Review 8.  Acetaminophen-induced Liver Injury: from Animal Models to Humans.

Authors:  Hartmut Jaeschke; Yuchao Xie; Mitchell R McGill
Journal:  J Clin Transl Hepatol       Date:  2014-09-15

9.  ADHD-associated dopamine transporter, latrophilin and neurofibromin share a dopamine-related locomotor signature in Drosophila.

Authors:  M van der Voet; B Harich; B Franke; A Schenck
Journal:  Mol Psychiatry       Date:  2015-05-12       Impact factor: 15.992

Review 10.  Zebrafish as model organisms for studying drug-induced liver injury.

Authors:  A D Bastiaan Vliegenthart; Carl S Tucker; Jorge Del Pozo; James W Dear
Journal:  Br J Clin Pharmacol       Date:  2014-12       Impact factor: 4.335

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3.  Pharmacological analysis of zebrafish lphn3.1 morphant larvae suggests that saturated dopaminergic signaling could underlie the ADHD-like locomotor hyperactivity.

Authors:  Merlin Lange; Cynthia Froc; Hannah Grunwald; William H J Norton; Laure Bally-Cuif
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4.  Acetaminophen Disrupts the Development of Pharyngeal Arch-Derived Cartilage and Muscle in Zebrafish.

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