Conducting bioinformatics analysis to predict sulforaphane-triggered adverse outcome pathways in healthy human cells - 26/02/23
, Katarina Živančević a, b, Katarina Baralić a, Evica Antonijević Miljaković a, Aleksandra Buha Djordjević a, Marijana Ćurčić a, Zorica Bulat a, Biljana Antonijević a, Danijela Đukić-Ćosić aAbstract |
Sulforaphane (SFN) is a naturally occurring molecule present in plants from Brassica family. It becomes bioactive after hydrolytic reaction mediated by myrosinase or human gastrointestinal microbiota. Sulforaphane gained scientific popularity due to its antioxidant and anti-cancer properties. However, its toxicity profile and potential to cause adverse effects remain largely unidentified. Thus, this study aimed to generate SFN-triggered adverse outcome pathway (AOP) by looking at the relationship between SFN-chemical structure and its toxicity, as well as SFN-gene interactions. Quantitative structure-activity relationship (QSAR) analysis identified 2 toxophores (Derek Nexus software) that have the potential to cause chromosomal damage and skin sensitization in mammals or mutagenicity in bacteria. Data extracted from Comparative Toxicogenomics Database (CTD) linked SFN with previously proposed outcomes via gene interactions. The total of 11 and 146 genes connected SFN with chromosomal damage and skin diseases, respectively. However, network analysis (NetworkAnalyst tool) revealed that these genes function in wider networks containing 490 and 1986 nodes, respectively. The over-representation analysis (ExpressAnalyst tool) pointed out crucial biological pathways regulated by SFN-interfering genes. These pathways are uploaded to AOP-helpFinder tool which found the 2321 connections between 19 enriched pathways and SFN which were further considered as key events. Two major, interconnected AOPs were generated: first starting from disruption of biological pathways involved in cell cycle and cell proliferation leading to increased apoptosis, and the second one connecting activated immune system signaling pathways to inflammation and apoptosis. In both cases, chromosomal damage and/or skin diseases such as dermatitis or psoriasis appear as adverse outcomes.
Il testo completo di questo articolo è disponibile in PDF.Graphical Abstract |
Highlights |
• | SFN contains 2 toxophores: isocyanate and isothiocyante. |
• | SFN could induce: skin sensitization and chromosomal damage in mammals as AOs. |
• | 11 and 146 SFN-related genes linked to chromosomal damage and skin diseases, respectively. |
• | SFN-triggered PPI networks of 490 and 1986 proteins are linked to chromosomal damage or skin diseases. |
• | SFN triggered KE: cell cycle disruption, apoptosis and immune system activation. |
Keywords : Sulforaphane, Adverse outcome pathway, Toxicology systems approach, Skin diseases, Chromosomal damage
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Vol 160
Articolo 114316- aprile 2023 Ritorno al numero
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