Proteomics

Dataset Information

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Determination of the mechanisms of hepatotoxicity induced by chlordecone and chlordecol from HepaRG cells and proteomic analyzes


ABSTRACT: Chlordecone (CLD) is a pesticide used to control the banana weevill in the French West Indies from 1970 to 1993. Despite its ban in the 90s, the highly persistence of CLD and contamination of the food webs raised tremendous concern for public health [1]. CLD can induce reprotoxic, neurotoxic and hepatotoxic effects in humans and is involved in prostate cancer [2] and liver fibrosis potentiation [3]. In liver, although CLD is metabolized into phase I metabolite chlordecol (CLD-OH), it is highly biopersistent. Nevertheless, the cellular hepatic effects of these 2 compounds have been poorly described. Therefore, we used an original approach to investigate in vitro toxicity responses of CLD and CLD-OH in liver cell models (HepaRG cells and primary human hepatocytes, PHHs) using metabolomics and proteomics. 1) Resiere, D., et al. (2023). Chlordecone (Kepone) poisoning in the French Territories in the Americas. Lancet 401, 916. 2) Multigner L., et al. (2010). Chlordecone exposure and risk of prostate cancer. J Clin Oncol 28, 3457-3462. 3) Tabet E., et al. (2016). Chlordecone potentiates hepatic fibrosis in chronic liver injury induced by carbon tetrachloride in mice. Toxicol Lett 255, 1-10.

INSTRUMENT(S): Q Exactive Plus

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Hepatocyte, Cell Culture

SUBMITTER: Thibaut LEGER  

LAB HEAD: Thibaut Léger

PROVIDER: PXD043683 | Pride | 2025-06-10

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
131222-degradation-proteomics-CLD-CLDOH-Perseus.txt Txt
161122-kinetic-CLD-CLDOH-Perseus.txt Txt
270122-dose-response-CLD-CLDOH-Perseus.txt Txt
BAF-01.mgf Mgf
BAF-01.raw Raw
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Publications

Fate and PPARγ and STATs-driven effects of the mitochondrial complex I inhibitor tebufenpyrad in liver cells revealed with multi-omics.

Léger Thibaut T   Balaguer Patrick P   Le Hégarat Ludovic L   Fessard Valérie V  

Journal of hazardous materials 20220929


The biological effects of the pesticide and mitochondrial complex I inhibitor tebufenpyrad (TEBU) on liver cells were investigated by combining proteomics and metabolomics. Both cell culture media and cellular lysates were analyzed in dose-response and kinetic experiments on the HepaRG cell line. Responses were compared with those obtained on primary human and rat hepatocytes. A multitude of phase I and II metabolites (>80) mainly common to HepaRG cells and primary hepatocytes and an increase in  ...[more]