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基于代谢组学和蛋白质基因组学联合方法探究卡马西平、双氯芬酸和文拉法辛对贻贝的混合物效应。

Mixture effects of pharmaceuticals carbamazepine, diclofenac and venlafaxine on Mytilus galloprovincialis mussel probed by metabolomics and proteogenomics combined approach.

机构信息

HydroSciences Montpellier, IRD, CNRS, University of Montpellier, Montpellier, France.

School of Pharmaceutical Sciences, University of Geneva, Geneva 1211, Switzerland; Institute of Pharmaceutical Sciences of Western Switzerland, University of Geneva, Geneva 1211, Switzerland.

出版信息

Sci Total Environ. 2024 Jan 10;907:168015. doi: 10.1016/j.scitotenv.2023.168015. Epub 2023 Oct 23.

DOI:10.1016/j.scitotenv.2023.168015
PMID:37879482
Abstract

Exposure to single molecules under laboratory conditions has led to a better understanding of the mechanisms of action (MeOAs) and effects of pharmaceutical active compounds (PhACs) on non-target organisms. However, not taking the co-occurrence of contaminants in the environment and their possible interactions into account may lead to underestimation of their impacts. In this study, we combined untargeted metabolomics and proteogenomics approaches to assess the mixture effects of diclofenac, carbamazepine and venlafaxine on marine mussels (Mytilus galloprovincialis). Our multi-omics approach and data fusion strategy highlighted how such xenobiotic cocktails induce important cellular changes that can be harmful to marine bivalves. This response is mainly characterized by energy metabolism disruption, fatty acid degradation, protein synthesis and degradation, and the induction of endoplasmic reticulum stress and oxidative stress. The known MeOAs and molecular signatures of PhACs were taken into consideration to gain insight into the mixture effects, thereby revealing a potential additive effect. Multi-omics approaches on mussels as sentinels offer a comprehensive overview of molecular and cellular responses triggered by exposure to contaminant mixtures, even at environmental concentrations.

摘要

在实验室条件下接触单个分子,可以更好地了解药物活性化合物(PhACs)对非靶标生物的作用机制(MeOAs)和影响。然而,如果不考虑环境中污染物的共同存在及其可能的相互作用,可能会低估它们的影响。在这项研究中,我们结合了非靶向代谢组学和蛋白质基因组学方法来评估二氯芬酸、卡马西平和文拉法辛对海洋贻贝(贻贝)的混合物效应。我们的多组学方法和数据融合策略突出了这种外源性鸡尾酒如何诱导可能对海洋双壳类动物有害的重要细胞变化。这种反应主要表现为能量代谢紊乱、脂肪酸降解、蛋白质合成和降解,以及内质网应激和氧化应激的诱导。考虑到已知的 PhACs 的 MeOAs 和分子特征,我们深入了解了混合物的作用,从而揭示了一种潜在的加性效应。贻贝作为哨兵的多组学方法提供了对暴露于污染物混合物引发的分子和细胞反应的全面概述,即使在环境浓度下也是如此。

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