Assessment of Pre- and Pro-haptens Using Nonanimal Test Methods for Skin Sensitization

Urbisch, Daniel; Becker, Matthias; Honarvar, Naveed; Kolle, Susanne N.; Mehling, Annette; Teubner, Wera; Wareing, Britta; Landsiedel, Robert

doi:10.1021/acs.chemrestox.6b00055

Cited by 56 publications

(42 citation statements)

References 41 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Similar chemical effects (oxidation of weakly reactive chemicals) can be induced by cytochrome P450, although the activity of these enzymes in human skin is not very high . Of the fragrance compounds studied here, citral, d ‐limonene and linalool were found to be prehaptens, eugenol and isoeugenol are prohaptens, and cinnamyl alcohol and geraniol are both prehaptens and prohaptens . In agreement with these observations, recent experiments showed that benzyl benzoate, benzyl salicylate and benzyl cinnamate remained chemically stable when exposed to forced degradation by oxidation, and remained non‐reactive to cysteine .…”

Section: Discussionsupporting

confidence: 87%

Molecular docking predictions of fragrance binding to human leukocyte antigen molecules

Schutte

Zhang

et al. 2019

Contact Dermatitis

View full text Add to dashboard Cite

Background: Over 4000 small chemicals have been identified as allergens capable of inducing skin sensitization. Many sensitizers are hypothesized to act as haptens producing novel antigens, which can be presented to T cells by human leukocyte antigens (HLAs). Recent studies suggest that some chemical allergens use haptenindependent mechanisms.Objective: To determine whether molecular docking can identify HLA molecules that bind skin-sensitizing chemical allergens.Methods: Structural models of HLA molecules were used as the basis for molecular docking of 22 chemical allergens. Allergens predicted to bind HLA-B*57:01 were tested for their ability to stimulate T cells by the use of proliferation and interferongamma enzyme-linked immunospot assays.

show abstract

Section: Discussionsupporting

confidence: 87%

Molecular docking predictions of fragrance binding to human leukocyte antigen molecules

Schutte

Zhang

et al. 2019

Contact Dermatitis

View full text Add to dashboard Cite

show abstract

“…Chemicals identified as Michael acceptors or S N 2 electrophiles have an excellent probability of having their sensitization potential predicted correctly. This fits with what is currently known about the ability of the non-animal assays leading into the network; mainly that the DPRACys and KeratinoSens™ assays tend to work best with soft electrophiles [38]. While LLNA class prediction was poor for those with an S N 2 domain, it was excellent for Michael acceptors at 76 86 66 %, i.e.…”

Section: Local Validity Analysissupporting

confidence: 82%

Application of IATA – A case study in evaluating the global and local performance of a Bayesian network model for skin sensitization

Fitzpatrick

Patlewicz

2017

SAR and QSAR in Environmental Research

View full text Add to dashboard Cite

The information characterizing key events in an Adverse Outcome Pathway (AOP) can be generated from in silico, in chemico, in vitro and in vivo approaches. Integration of this information and interpretation for decision making are known as integrated approaches to testing and assessment (IATA). One such IATA was published by Jaworska et al., which describes a Bayesian network model known as ITS-2. The current work evaluated the performance of ITS-2 using a stratified cross-validation approach. We also characterized the impact of replacing the most significant component of the network, output from the expert system TIMES-SS, with structural alert information from the OECD Toolbox and Toxtree. Lack of structural alerts or TIMES-SS predictions yielded a sensitization potential prediction of 79%. If the TIMES-SS prediction was replaced by a structural alert indicator, the network predictivity increased up to 87%. The original network's predictivity was 89%. The local applicability domain of the original ITS-2 network was also evaluated using reaction mechanistic domains to understand what types of chemicals ITS-2 was able to make the best predictions for. We found that the original network was successful at predicting which chemicals would be sensitizers, but not at predicting their potency.

show abstract

“…using the available methods show limitations in the demonstration of concentration-dependency and have limited capacities to detect certain prohaptens and for potency prediction (Piroird et al, 2015;Natsch et al, 2015;Nukada et al, 2012;Teunis et al, 2014;Jaworska et al, 2015;Urbisch et al, 2016;Adler et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

Keratinocytes improve prediction of sensitization potential and potency of chemicals with THP-1 cells_suppl

Hennen

2017

ALTEX

View full text Add to dashboard Cite

Quantitative data on sensitization potency of chemicals has long been derived from in vivo data obtained with the local lymph node assay (LLNA) in mice. The minimum concentration of a chemical that can induce a sensitization response, i.e. the chemical's sensitization potency, is an essential value in quantitative risk assessment (Mackay et al., 2013). In vitro methods intended to reduce or replace animal testing in this area need to be able to predict hazard and also to categorize the potency of sensitizers.We and others have shown sensitizer-induced CD86 and CD54 upregulation on monocytic THP-1 cells as a model for DC activation (Bocchietto et al., 2007;Goebel et al., 2014;Krutz et al., 2015;Tietze and Blömeke, 2008;Yoshida et al., 2003). However, the impact of the presence of keratinocytes on the activation of THP-1 cells has not yet been fully investigated.In this study, we used our HaCaT/THP-1 coculture setup (Hennen et al., 2011) to study the impact of keratinocytes on the expression of CD86 and CD54 on THP-1 after treatment with a set of 14 sensitizers and 10 non-sensitizers: We evaluated (1) the magnitude of CD86 and CD54 upregulation in the coculture model in comparison to THP-1 monoculture, (2) the sensitivity, specificity and accuracy of the HaCaT/THP-1 coculture model to IntroductionThe hallmarks of chemical sensitizers are their ability to form antigenic haptenated proteins, to induce inflammatory responses in keratinocytes, and to induce maturation of dendritic cells (DC) needed for efficient activation of naïve T cells (OECD, 2012).DC activation by sensitizers causes the upregulation of costimulatory molecules such as CD86 (Linsley et al., 1991), CD54 (Grakoui et al., 1999;Comrie et al., 2015), and other surface molecules (reviewed by Hubo et al., 2013) that are involved in antigen presentation. After interaction with their counterparts on T cells, these surface molecules generate a costimulatory signal (signal 2) that synergizes with the T cell receptor-mediated signal (signal 1) to promote an adaptive immune response.Keratinocytes exposed to sensitizers release proinflammatory or immunomodulatory cytokines (Gober and Gaspari, 2008;Pasparakis et al., 2014). These factors can trigger DC activation and/or DC mobilization (reviewed by Kaplan et al., 2012). This role of adjacent keratinocytes may therefore have a significant impact on the strength of the chemical-induced DC response. Accordingly, we postulated that keratinocytes impact on the quantitative response of DC to skin sensitizing chemicals. Research Article Keratinocytes Improve Prediction of Sensitization Potential and Potency of Chemicals with THP-1 Cells Jennifer Hennen and Brunhilde BlömekeDepartment of Environmental Toxicology, Trier University, Trier, Germany SummaryIn vitro approaches to address key steps of chemical-induced skin sensitization have been developed, but there is uncertainty how keratinocytes, which play a crucial role not only regarding xenobiotic metabolism but also skin inflammation, impact on a chemical's potential ...

show abstract

Assessment of Pre- and Pro-haptens Using Nonanimal Test Methods for Skin Sensitization

Cited by 56 publications

References 41 publications

Molecular docking predictions of fragrance binding to human leukocyte antigen molecules

Molecular docking predictions of fragrance binding to human leukocyte antigen molecules

Application of IATA – A case study in evaluating the global and local performance of a Bayesian network model for skin sensitization

Keratinocytes improve prediction of sensitization potential and potency of chemicals with THP-1 cells_suppl

Contact Info

Product

Resources

About