Substantiate a read-across hypothesis by using transcriptome data-A case study on volatile diketones

Christina Drake; Matthias M Wehr; Walter Zobl; Jeannette Koschmann; David De Lucca; Britta A Kühne; Tanja Hansen; Jan Knebel; Detlef Ritter; Jan Boei; Harry Vrieling; Annette Bitsch; Sylvia E Escher

doi:10.3389/ftox.2023.1155645

Substantiate a read-across hypothesis by using transcriptome data-A case study on volatile diketones

Front Toxicol. 2023 May 3:5:1155645. doi: 10.3389/ftox.2023.1155645. eCollection 2023.

Authors

Affiliations

¹ Fraunhofer Institute for Toxicology and Experimental Medicine, Chemical Safety and Toxicology, Hannover, Germany.
² GeneXplain GmbH, Wolfenbüttel, Germany.
³ Medizinische Hochschule Hannover, Hannover, Germany.
⁴ Leiden University Medical Center, Leiden, Netherlands.

Abstract

This case study explores the applicability of transcriptome data to characterize a common mechanism of action within groups of short-chain aliphatic α-, β-, and γ-diketones. Human reference in vivo data indicate that the α-diketone diacetyl induces bronchiolitis obliterans in workers involved in the preparation of microwave popcorn. The other three α-diketones induced inflammatory responses in preclinical in vivo animal studies, whereas beta and gamma diketones in addition caused neuronal effects. We investigated early transcriptional responses in primary human bronchiolar (PBEC) cell cultures after 24 h and 72 h of air-liquid exposure. Differentially expressed genes (DEGs) were assessed based on transcriptome data generated with the EUToxRisk gene panel of Temp-O-Seq^®. For each individual substance, genes were identified displaying a consistent differential expression across dose and exposure duration. The log fold change values of the DEG profiles indicate that α- and β-diketones are more active compared to γ-diketones. α-diketones in particular showed a highly concordant expression pattern, which may serve as a first indication of the shared mode of action. In order to gain a better mechanistic understanding, the resultant DEGs were submitted to a pathway analysis using ConsensusPathDB. The four α-diketones showed very similar results with regard to the number of activated and shared pathways. Overall, the number of signaling pathways decreased from α-to β-to γ-diketones. Additionally, we reconstructed networks of genes that interact with one another and are associated with different adverse outcomes such as fibrosis, inflammation or apoptosis using the TRANSPATH-database. Transcription factor enrichment and upstream analyses with the geneXplain platform revealed highly interacting gene products (called master regulators, MRs) per case study compound. The mapping of the resultant MRs on the reconstructed networks, visualized similar gene regulation with regard to fibrosis, inflammation and apoptosis. This analysis showed that transcriptome data can strengthen the similarity assessment of compounds, which is of particular importance, e.g., in read-across approaches. It is one important step towards grouping of compounds based on biological profiles.

Keywords: PBEC; TempO-seq; new approach methodology; protein network analysis; read across; transcriptomics.

Grants and funding

This work has received funding from the European Union’s Horizon 2020 research and innovation program under grant agreements No. 681002 (EU-ToxRisk), No. 964537 (RISK-HUNT3R) and by the Ministry of Science and Culture of the State Lower Saxony (Germany) through the project FibrOmics.