Luz Anthony L, Kassotis Christopher D, Stapleton Heather M, Meyer Joel N
Nicholas School of the Environment, Box 90328, Duke University, Durham, NC, 27708, USA.
Toxicology. 2018 Jan 15;393:150-159. doi: 10.1016/j.tox.2017.11.010. Epub 2017 Nov 7.
Pyraclostrobin is one of the most heavily used fungicides, and has been detected on a variety of produce, suggesting human exposure occurs regularly. Recently, pyraclostrobin exposure has been linked to a variety of toxic effects, including neurodegeneration and triglyceride (TG) accumulation. As pyraclostrobin inhibits electron transport chain complex III, and as mitochondrial dysfunction is associated with metabolic syndrome (cardiovascular disease, type II diabetes, obesity), we designed experiments to test the hypothesis that mitochondrial dysfunction underlies its adipogenic activity. 3T3-L1 cells were differentiated according to standard protocols in the presence of pyraclostrobin, resulting in TG accumulation. However, TG accumulation occurred without activation of the peroxisome proliferator activated nuclear receptor gamma (PPARγ), the canonical pathway mediating adipogenesis. Furthermore, cells failed to express many markers of adipogenesis (PPARγ, lpl, CEBPα), while co-exposure to pyraclostrobin and two different PPARγ antagonists (GW9662, T0070907) failed to mitigate TG accumulation, suggesting TG accumulation occurred through a PPARγ-independent mechanism. Instead, pyraclostrobin reduced steady-state ATP, mitochondrial membrane potential, basal mitochondrial respiration, ATP-linked respiration, and spare respiratory capacity, demonstrating mitochondrial dysfunction, while reduced expression of genes involved in glucose transport (Glut-4), glycolysis (Pkm, Pfkl, Pfkm), fatty acid oxidation (Cpt-1b), and lipogenesis (Fasn, Acacα, Acacβ) further suggested a disruption of metabolism. Finally, inhibition of cAMP responsive element binding protein (CREB), a PPARγ coactivator, partially mitigated pyraclostrobin-induced TG accumulation, suggesting TG accumulation is occurring through a CREB-driven mechanism. In contrast, rosiglitazone, a known PPARγ agonist, induced TG accumulation in a PPARγ-dependent manner and enhanced mitochondrial function. Collectively, these results suggest pyraclostrobin-induced mitochondrial dysfunction inhibits lipid homeostasis, resulting in TG accumulation. Exposures that disrupt mitochondrial function may have the potential to contribute to the rising incidence of metabolic syndrome, and thus more research is needed to understand the human health impact of pyraclostrobin exposure.
吡唑醚菌酯是使用最为广泛的杀菌剂之一,已在多种农产品中被检测到,这表明人类经常接触到该物质。最近,接触吡唑醚菌酯与多种毒性作用有关,包括神经退行性变和甘油三酯(TG)蓄积。由于吡唑醚菌酯会抑制电子传递链复合物III,且线粒体功能障碍与代谢综合征(心血管疾病、II型糖尿病、肥胖症)相关,我们设计了实验来验证线粒体功能障碍是其促脂肪生成活性基础这一假设。3T3-L1细胞在吡唑醚菌酯存在的情况下按照标准方案进行分化,导致TG蓄积。然而,TG的蓄积并未伴随着过氧化物酶体增殖物激活受体γ(PPARγ)的激活,而PPARγ是介导脂肪生成的经典途径。此外,细胞未能表达许多脂肪生成标志物(PPARγ、脂蛋白脂肪酶、CCAAT增强子结合蛋白α),同时,将吡唑醚菌酯与两种不同的PPARγ拮抗剂(GW9662、T0070907)共同作用并不能减轻TG的蓄积,这表明TG的蓄积是通过一种不依赖PPARγ的机制发生的。相反,吡唑醚菌酯降低了稳态ATP、线粒体膜电位、基础线粒体呼吸、ATP相关呼吸和备用呼吸能力,表明存在线粒体功能障碍,而参与葡萄糖转运(Glut-4)、糖酵解(丙酮酸激酶、磷酸果糖激酶1、磷酸果糖激酶M)、脂肪酸氧化(肉碱/有机阳离子转运体1b)和脂肪生成(脂肪酸合酶、乙酰辅酶A羧化酶α、乙酰辅酶A羧化酶β)的基因表达降低,进一步表明代谢受到了干扰。最后,抑制cAMP反应元件结合蛋白(CREB)(一种PPARγ共激活因子)可部分减轻吡唑醚菌酯诱导的TG蓄积,这表明TG的蓄积是通过一种由CREB驱动的机制发生的。相比之下,罗格列酮是一种已知的PPARγ激动剂,它以PPARγ依赖的方式诱导TG蓄积并增强线粒体功能。总的来说,这些结果表明吡唑醚菌酯诱导的线粒体功能障碍会抑制脂质稳态,导致TG蓄积。破坏线粒体功能的接触可能会导致代谢综合征发病率上升,因此需要更多的研究来了解接触吡唑醚菌酯对人类健康的影响。