Toxicological risks of SDHIs and QoIs to zebrafish (Danio rerio) and the corresponding poisoning mechanism.

Quinone outside inhibitor fungicides (QoIs) and succinate dehydrogenase inhibitor fungicides (SDHIs) were classified as highly or moderately toxic to nontarget aquatic organisms, which deterred their application in paddy scenario. Currently, the mechanism of toxicity regarding which factors govern their risk ranking in fish species are not fully explored. In this study, adult zebrafish were exposed to four QoIs (pyraclostrobin, trifloxystrobin, kresoxim-methyl, and azoxystrobin) and three SDHIs (isopyrazam, thifluzamide, and boscalid) to assess its acute toxicity and effects on tissue accumulation and gill injury. The results showed that the overall toxicity level was in the order of QoIs > SDHIs, whereas the order of accumulation capacity was SDHIs > QoIs. Seven mitochondrial respiratory inhibitors exposure induced serious histological damage in the gills, including aneurism, curling, telangiectasia and swelling, and caused mitochondrial dysfunction and weaker complex II and III activities. The correlation between their acute toxicities and in vitro gill cytotoxicity was significant (R = 0.868), whereas the bioaccumulation level was not markedly associated with their 96h-LC values in zebrafish (R = -0.686), indicating the degree of target organ (gill) injury may be the decisive factor that governs the risk grade of respiratory inhibitors in fish. Additionally, the docking positions and binding energies of fungicides with the target proteins may be responsible for their differential branchial damage. These results offer a point of reference and theoretical support for the design of fungicides and appropriate formulations with improved environmental safety that could broaden their application scenario.