Author Contributions

Front. Toxicol.

Frontiers in Toxicology

Front. Toxicol.

2673-3080

Frontiers Media S.A.

10.3389/ftox.2020.00003

Toxicology

Specialty Grand Challenge

A Brainer on Neurotoxicity

Fritsche

Ellen

¹ ² ^* Hogberg

Helena Therese

³ ^*

¹IUF-Leibniz Research Institute for Environmental Medicine, Düsseldorf, Germany ²Medical Faculty, Heinrich-Heine-University, Düsseldorf, Germany ³Center for Alternatives to Animal Testing (CAAT) at the Johns Hopkins Bloomberg School of Public Health, Baltimore, MD, United States

Edited by: Timothy J. Shafer, United States Environmental Protection Agency (EPA), United States

Reviewed by: David M. Reif, North Carolina State University, United States; Anke Marije Tukker, Utrecht University, Netherlands

*Correspondence: Ellen Fritsche ellen.fritsche@iuf-duesseldorf.de Helena Therese Hogberg hhogber2@jhu.edu

This article was submitted to Neurotoxicology, a section of the journal Frontiers in Toxicology

30 06 2020

2020

19 05 2020 11 06 2020

2020

Fritsche and Hogberg

This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

neurotoxicity DNT human relevance developmental neurotoxicity susceptible life stages

We talk about adult neurotoxicity when exposure to natural or manmade toxic substances, interferes with normal nervous system activity and function. Neurotoxicity might disrupt or even kill neurons or the surrounding glia cells by interfering with neural function. Special attention must be given to susceptible subgroups such as, the very young (developmental neurotoxicity - DNT) and the aging population, as neurotoxicity's mode-of-action (MoA) or sensitivity differs for them vs. healthy adults. So far, neurotoxicity has been evaluated using animal models, rodent primary, or tumor in vitro cultures, and human epidemiology.

The field of neurotoxicology has benefitted tremendously from the field of drug development for nervous system disorders. High attrition rates, (at least 50%) in general (Smietana et al., 2016) and for central nervous system (CNS) drugs specifically (Arrowsmith and Miller, 2013; DiMasi, 2014; Harrison, 2016; Mohs and Greig, 2017), were attributed to insufficient human predictability of nonclinical biological data, i.e., efficacy and safety issues (Bailey et al., 2014; DiMasi, 2014; Harrison, 2016; Cavero et al., 2019). For CNS drug development, transgenic animals modeling human disease are widely used. The especially high failure rate of CNS drug developments is ascribed amongst others to the complexity of human CNS diseases that often involve multiple molecular targets. Furthermore, experimental animal disease models have relatively low predictive validity, and there is lack of established clinical biomarkers and proof-of-concept models for these diseases (Kola and Landis, 2004; Palmer and Stephenson, 2005). The failure rate in clinical trials is especially high for neurodegenerative disorders such as Alzheimer disease where 99.6% of drugs do not make it to the market (Pistollato et al., 2016; Mohs and Greig, 2017). Including human-relevant pharmacokinetics and bioavailability early into the drug development phase already reduced drug failure rates (Kola and Landis, 2004). Hence, improvement of the pharmaco-/toxicodynamics of models in health and disease for predicting not only drug effects but also the neurotoxicity of environmental chemicals, particulate matter, or other noxae will aid the development of better human prediction (Leist and Hartung, 2013; Cavero et al., 2019).

It was in the year 1993 when the use of stem cells for toxicological research was first proposed. It took 10 more years to first involve mouse embryonic stem cells in neurotoxicity evaluation. In 2006, human-induced pluripotent stem cells (hiPSC) entered the field and were first applied for neurotoxicity evaluation in 2016 (Barenys and Fritsche, 2018). For over three decades, almost, toxicity in general as well as neurotoxicity evaluation have seen dramatic changes. A future was envisioned in which toxicology relied primarily on high-throughput in vitro assays and computational models based on human biology to evaluate potential adverse effects of chemical exposures in a regulatory context (NRC, 2007). Moreover, the value of exposure science and epidemiology was strongly recognized for achieving human-relevant risk assessment in the future (NRC, 2012, 2017). In the area of neurotoxicity, these novel concepts have specifically and systematically been taken up for DNT. A global scientific network has been aimed at setting up a DNT in vitro testing battery consisting of primarily human stem/progenitor cell-based assays as well as zebrafish—as an alternative model organism—with the ultimate goal of application for regulatory purposes (Lein et al., 2005; Bal-Price et al., 2015, 2018; Fritsche et al., 2017, 2018; OECD, 2020). In vitro methodologies for studying acute neurotoxicity have also seen rapid advancement. Reproducible production of electrically active human neurons in cultures has been achieved, and the transition from 2D to 3D methods allows us to obtain complex models suitable for investigating neurotoxicity or brain-related diseases also with patient-derived cells (Grainger et al., 2018; Yla-Outinen et al., 2019). Thus, human iPSC-derived cells offer a platform with the unique advantage of almost unlimited availability and reproducing the “human context” in vitro by preserving the genetic and molecular phenotype of their donors. Despite this, stem cells differentiated into neurons and astroglia, which have been the most common cell types used for neurotoxicity testing so far, do not solely represent the wholeness of a brain. Novel strategies, for example, implementing oligodendrocytes (Pamies et al., 2017, 2018), microglia (Abreu et al., 2018), region-specific astrocytes (de Majo et al., 2020), and vasculature (Worsdorfer et al., 2020) in standard neurotoxicity test methods, need more attention. In addition, while brain organoids offer much promise, there is a need to improve both the reproducibility and throughput of these models so that they can reach their full potential for neurotoxicity and DNT testing (Sivitilli et al., 2020).

The Specialty Section Neurotoxicology in the journal Frontiers in Toxicology will focus on ‘Human Relevance’ as an overarching theme. Papers are encouraged to deal with cutting-edge research in in vivo, in vitro, in silico, and in epidemiological approaches for neurotoxicity evaluation of all life stages. Primary research as well as review articles of all areas touching on neurotoxicological research are welcome. The human relevance of these findings needs to be discussed irrespective of the methods applied. Articles will target a broad audience including academic and clinical researchers as well as toxicologist from industry and regulatory agencies. Thus, the Specialty Section Neurotoxicology of Frontiers in Toxicology aims at generating a community for neurotoxicologists worldwide.

Author Contributions

EF and HH wrote the manuscript. All authors contributed to the article and approved the submitted version.

Conflict of Interest

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

References Abreu

C. M.

Gama

Krasemann

Chesnut

Odwin-Dacosta

Hogberg

H. T.

. (2018). Microglia increase inflammatory responses in iPSC-derived human BrainSpheres. Front. Microbiol. 9:2766. 10.3389/fmicb.2018.02766

30619100

Arrowsmith

Miller

(2013). Trial watch: phase II and phase III attrition rates 2011-2012. Nat. Rev. Drug Discov. 12:569. 10.1038/nrd4090

23903212

Bailey

Thew

Balls

(2014). An analysis of the use of animal models in predicting human toxicology and drug safety. Altern. Lab. Anim. 42, 181–199. 10.1177/026119291404200306

25068930

Bal-Price

Crofton

K. M.

Leist

Allen

Arand

Buetler

. (2015). International STakeholder NETwork (ISTNET): creating a developmental neurotoxicity (DNT) testing road map for regulatory purposes. Arch. Toxicol. 89, 269–287. 10.1007/s00204-015-1464-2

25618548

Bal-Price

Hogberg

H. T.

Crofton

K. M.

Daneshian

FitzGerald

R. E.

Fritsche

. (2018). Recommendation on test readiness criteria for new approach methods in toxicology: exemplified for developmental neurotoxicity. ALTEX 35, 306–352. 10.14573/altex.1712081

29485663

Barenys

Fritsche

(2018). A historical perspective on the use of stem/progenitor cell-based in vitro methods for neurodevelopmental toxicity testing. Toxicol. Sci. 165, 10–13. 10.1093/toxsci/kfy170

30325470

Cavero

Guillon

J. M.

Holzgrefe

H. H.

(2019). Human organotypic bioconstructs from organ-on-chip devices for human-predictive biological insights on drug candidates. Expert Opin. Drug Saf. 18, 651–677. 10.1080/14740338.2019.1634689

31268355

de Majo

Koontz

Rowitch

Ullian

E. M.

(2020). An update on human astrocytes and their role in development and disease. Glia 68, 685–704. 10.1002/glia.23771

31926040

DiMasi

J. A.

(2014). CNS Drugs Take Longer to Develop and Have Lower Success Rates Than Other Drugs. Tufts Center for the Study of Drug Development. Available online at: http://csdd.tufts.edu/. Fritsche

Barenys

Klose

Masjosthusmann

Nimtz

Schmuck

. (2018). Current availability of stem cell-based in vitro methods for developmental neurotoxicity (DNT) Testing. Toxicol. Sci. 165, 21–30. 10.1093/toxsci/kfy178 Fritsche

Crofton

K. M.

Hernandez

A. F.

Hougaard Bennekou

Leist

Bal-Price

. (2017). OECD/EFSA workshop on developmental neurotoxicity (DNT): the use of non-animal test methods for regulatory purposes. Altex 34, 311–315. 10.14573/altex.1701171

28407175

Grainger

A. I.

King

M. C.

Nagel

D. A.

Parri

H. R.

Coleman

M. D.

Hill

E. J.

(2018). In vitro models for seizure-liability testing using induced pluripotent stem cells. Front. Neurosci. 12:590. 10.3389/fnins.2018.00590

30233290

Harrison

R. K.

(2016). Phase II and phase III failures: 2013-2015. Nat. Rev. Drug Discov. 15, 817–818. 10.1038/nrd.2016.184

27811931

Kola

Landis

(2004). Can the pharmaceutical industry reduce attrition rates? Nat. Rev. Drug Discov. 3, 711–715. 10.1038/nrd1470

15286737

Lein

Silbergeld

Locke

Goldberg

A. M.

(2005). In vitro and other alternative approaches to developmental neurotoxicity testing (DNT). Environ. Toxicol. Pharmacol. 19, 735–744. 10.1016/j.etap.2004.12.035

21783550

Leist

Hartung

(2013). Inflammatory findings on species extrapolations: humans are definitely no 70-kg mice. Arch. Toxicol. 87, 563–567. 10.1007/s00204-013-1038-0

23503654

Mohs

R. C.

Greig

N. H.

(2017). Drug discovery and development: Role of basic biological research. Alzheimers Dement 3, 651–657. 10.1016/j.trci.2017.10.005

29255791

NRC (2007). National Research Council: Toxicity Testing in the 21st Century a Vision and a Strategy. Washington, DC: National Academy Press. NRC (2012). National Research Council: Exposure Science in the 21st Century A Vision and a Strategy. Washington, DC: National Research Council NRC (2017). National Research Council: Using 21st Century Science to Improve Risk-Related Evaluations. Washington, DC: National Research Council. OECD (2020). Report of the OECD/EFSA Workshop On Developmental Neurotoxicity (DNT): The Use of Non-Animal Test Methods for Regulatory Purposes. Series on Testing and Assessment, Organisation for Economic Co-operation and Development. Available online at: http://www.oecd.org/officialdocuments/publicdisplaydocumentpdf/?cote=ENV/JM/MONO(2017)4anddocLanguage=En,2017.28407175 Palmer

A. M.

Stephenson

F. A.

(2005). CNS drug discovery: challenges and solutions. Drug News Perspect. 18, 51–57.15753976 Pamies

Barreras

Block

Makri

Kumar

Wiersma

. (2017). A human brain microphysiological system derived from induced pluripotent stem cells to study neurological diseases and toxicity. Altex 34, 362–376. 10.14573/altex.1609122

27883356

Pamies

Block

Lau

Gribaldo

Pardo

C. A.

Barreras

. (2018). Rotenone exerts developmental neurotoxicity in a human brain spheroid model. Toxicol. Appl. Pharmacol. 354, 101–114. 10.1016/j.taap.2018.02.003

29428530

Pistollato

Ohayon

E. L.

Lam

Langley

G. R.

Novak

T. J.

Pamies

. (2016). Alzheimer disease research in the 21st century: past and current failures, new perspectives and funding priorities. Oncotarget 7, 38999–39016. 10.18632/oncotarget.9175

27229915

Sivitilli

A. A.

Gosio

J. T.

Ghoshal

Evstratova

Trcka

Ghiasi

. (2020). Robust production of uniform human cerebral organoids from pluripotent stem cells. Life Sci. Alliance 3:707. 10.26508/lsa.202000707

32303588

Smietana

Siatkowski

Moller

(2016). Trends in clinical success rates. Nat. Rev. Drug Discov. 15, 379–380. 10.1038/nrd.2016.85

27199245

Worsdorfer

Takashi

Asahina

Sumita

Ergun

(2020). Do not keep it simple: recent advances in the generation of complex organoids. J. Neural Transm. 10.1007/s00702-020-02198-832385575. [Epub ahead of print]. Yla-Outinen

L. J.

Tanskanen

M. A.

Kapucu

F. E.

Hyysalo

A. J.

. (2019). Advances in human stem cell-derived neuronal cell culturing and analysis. Adv. Neurobiol. 22, 299–329. 10.1007/978-3-030-11135-9_13

31073942

Funding. This work (EF) was supported by the project CERST (Center for Alternatives to Animal Testing) of the Ministry for culture and science (MKW) of the State of North-Rhine Westphalia, Germany [file number 233-1.08.03.03-121972].