Identification Of Decrease In Tric Proteins As Novel Targets Of Alpha-Amanitin-Derived Hepatotoxicity By Comparative Proteomic Analysis In Vitro

TOXINS(2021)

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摘要
Alpha-amanitin (alpha-AMA) is a cyclic peptide and one of the most lethal mushroom amatoxins found in Amanita phalloides. alpha-AMA is known to cause hepatotoxicity through RNA polymerase II inhibition, which acts in RNA and DNA translocation. To investigate the toxic signature of alpha-AMA beyond known mechanisms, we used quantitative nanoflow liquid chromatography-tandem mass spectrometry analysis coupled with tandem mass tag labeling to examine proteome dynamics in Huh-7 human hepatoma cells treated with toxic concentrations of alpha-AMA. Among the 1828 proteins identified, we quantified 1563 proteins, which revealed that four subunits in the T-complex protein 1-ring complex protein decreased depending on the alpha-AMA concentration. We conducted bioinformatics analyses of the quantified proteins to characterize the toxic signature of alpha-AMA in hepatoma cells. This is the first report of global changes in proteome abundance with variations in alpha-AMA concentration, and our findings suggest a novel molecular regulation mechanism for hepatotoxicity.
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关键词
alpha-amanitin, comparative quantitative proteomics, TRiC, hepatotoxicity
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