Alternariol (AOH), alternariol monomethyl ether (AME), and tenuazonic acid (TeA) are three major emerging Alternaria toxins in food. In this lncRNA-mRNA omics-based study, we first decrypt the blueprint: how emerging Alternaria toxins induce hepatic stellate cell LX-2 transdifferentiation for liver fibrosis. AOH and AME caused the fibrotic marker α-smooth muscle actin, extracellular matrix collagen expression, and cell contraction, while TeA had no significant effect. Mechanistically, AOH, AME, and AAT (their combination) activated the NF-κB pathway and induced ferroptosis and AMPK/AKT/m-TOR-related autophagy. Meanwhile, lncRNAs associated with hepatotoxicity were analyzed, and core LncRNAs associated with transdifferentiation were identified. Furthermore, we also proposed a CotA degradation strategy to eliminate the AOH hepatotoxicity. In summary, the present study identifies the potential hepatotoxicity of Alternaria toxins, introduces a CotA laccase-mediated detoxification approach, and lays a foundation for subsequent research and control strategies targeting hepatotoxicity.
Lin et al. (Mon,) studied this question.