Limitations and Modifications of Skin Sensitization NAMs for Testing Inorganic Nanomaterials

Britta Wareing; Ayse Aktalay Hippchen; Susanne N. Kolle; Barbara Birk; Dorothee Funk-Weyer; Robert Landsiedel

doi:10.3390/toxics12080616

Toxics (Aug 2024)

Limitations and Modifications of Skin Sensitization NAMs for Testing Inorganic Nanomaterials

Britta Wareing,
Ayse Aktalay Hippchen,
Susanne N. Kolle,
Barbara Birk,
Dorothee Funk-Weyer,
Robert Landsiedel

Affiliations

Britta Wareing: BASF SE, Experimental Toxicology and Ecology, 67057 Ludwigshafen, Germany
Ayse Aktalay Hippchen: BASF SE, Experimental Toxicology and Ecology, 67057 Ludwigshafen, Germany
Susanne N. Kolle: BASF SE, Experimental Toxicology and Ecology, 67057 Ludwigshafen, Germany
Barbara Birk: BASF SE, Agriculture Solutions, 67117 Limburgerhof, Germany
Dorothee Funk-Weyer: BASF SE, Experimental Toxicology and Ecology, 67057 Ludwigshafen, Germany
Robert Landsiedel: BASF SE, Experimental Toxicology and Ecology, 67057 Ludwigshafen, Germany

DOI: https://doi.org/10.3390/toxics12080616
Journal volume & issue: Vol. 12, no. 8
p. 616

Abstract

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Since 2020, the REACh regulation requires toxicological data on nanoforms of materials, including the assessment of their skin-sensitizing properties. Small molecules’ skin sensitization potential can be assessed by new approach methodologies (NAMs) addressing three key events (KE: protein interaction, activation of dendritic cells, and activation of keratinocytes) combined in a defined approach (DA) described in the OECD guideline 497. In the present study, the applicability of three NAMs (DPRA, LuSens, and h-CLAT) to nine materials (eight inorganic nanomaterials (NM) consisting of CeO2, BaSO4, TiO2 or SiO2, and quartz) was evaluated. The NAMs were technically applicable to NM using a specific sample preparation (NANOGENOTOX dispersion protocol) and method modifications to reduce interaction of NM with the photometric and flowcytometric read-outs. The results of the three assays were combined according to the defined approach described in the OECD guideline No. 497; two of the inorganic NM were identified as skin sensitizers. However, data from animal studies (for ZnO, also human data) indicate no skin sensitization potential. The remaining seven test substances were assessed as “inconclusive” because all inorganic NM were outside the domain of the DPRA, and the achievable test concentrations were not sufficiently high according to the current test guidelines of all three NAMs. The use of these NAMs for (inorganic) NM and the relevance of the results in general are challenged in three ways: (i) NAMs need modification to be applicable to insoluble, inorganic matter; (ii) current test guidelines lack adequate concentration metrics and top concentrations achievable for NM; and (iii) NM may not cause skin sensitization by the same molecular and cellular key events as small organic molecules do; in fact, T-cell-mediated hypersensitivity may not be the most relevant reaction of the immune system to NM. We conclude that the NAMs adopted by OECD test guidelines are currently not a good fit for testing inorganic NM.

Published in Toxics

ISSN: 2305-6304 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Technology: Chemical technology
Website: http://www.mdpi.com/journal/toxics/

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