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Evaluation of in vitro assays for the assessment of the skin sensitization hazard of functional polysiloxanes and silanes

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Abstract The skin sensitization potential of chemicals has traditionally been evaluated in vivo according to OECD testing guidelines in guinea pigs or the mouse local lymph node assay. There has… Click to show full abstract

Abstract The skin sensitization potential of chemicals has traditionally been evaluated in vivo according to OECD testing guidelines in guinea pigs or the mouse local lymph node assay. There has lately been a great emphasis on establishing in vitro test methods reflecting the key biological events in the adverse outcome pathway (AOP) for skin sensitization as published by the OECD. Against this background, a group of 8 polysiloxanes and silanes, seven of them aminofunctionalised, for which in vivo data were already available, has been tested in vitro in the direct peptide reactivity assay (DPRA), the KeratinoSens™ and the human cell line activation test (h‐CLAT) and in the modified myeloid U937 skin sensitization test (mMUSST) as far as technically feasible. The main objective of the programme was to determine the utility of these systems for this heterogeneous group of silicone‐based substances, recognizing that some substances are outside the assays applicability domains. The presented data provided some interesting mechanistical insights into the performance of these assays for functionalised siloxanes and silanes. The data also allow for a preliminary evaluation of proposed integrated testing strategies (ITS) to determine the skin sensitization potential of chemicals which were not considered in the training sets of the respective ITS. HighlightsIndividual assays produced heterogeneous, often false negative results.Assay's metabolic capacity appears to play a critical roleh‐CLAT appears less suitable compared to the mMUSST assay for aminofunctional polysiloxanes and silanes.Applying ‘2 out of 3’ ITS provides mixed results.

Keywords: evaluation vitro; sensitization; skin sensitization; polysiloxanes silanes

Journal Title: Regulatory Toxicology and Pharmacology
Year Published: 2017

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