AI Article Synopsis

  • Chemical proteomics can identify novel protein targets for small molecules, but validating these targets can be difficult due to the sheer number generated.
  • This study integrated various methods, including cellular thermal shift assay (CETSA) and mass spectrometry, to identify 74 protein targets of the environmental toxicant monoethylhexyl phthalate (MEHP).
  • The findings suggest that MEHP induces cell cycle dysregulation, specifically causing hepatocytes to arrest at the G1 stage, and identified key regulatory proteins (CPEB4, ANAPC5, and SPOUT1) as significant targets.

Article Abstract

Chemical proteomics methods have been used as effective tools to identify novel protein targets for small molecules. These methods have great potential to be applied as environmental toxicants to figure out their mode of action. However, these assays usually generate dozens of possible targets, making it challenging to validate the most important one. In this study, we have integrated the cellular thermal shift assay (CETSA), quantitative proteomics, metabolomics, computer-assisted docking, and target validation methods to uncover the protein targets of monoethylhexyl phthalate (MEHP). Using the mass spectrometry implementation of CETSA (MS-CETSA), we have identified 74 possible protein targets of MEHP. The Gene Ontology (GO) enrichment integration was further conducted for the target proteins, the cellular dysregulated proteins, and the metabolites, showing that cell cycle dysregulation could be one primary change due to the MEHP-induced toxicity. Flow cytometry analysis confirmed that hepatocytes were arrested at the G1 stage due to the treatment with MEHP. Subsequently, the potential protein targets were ranked by their binding energy calculated from the computer-assisted docking with MEHP. In summary, we have demonstrated the development of interactomics workflow to simplify the redundant information from multiomics data and identified novel cell cycle regulatory protein targets (CPEB4, ANAPC5, and SPOUT1) for MEHP.

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Source
http://dx.doi.org/10.1021/acs.est.0c05832DOI Listing

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