Toxic effects of Cr(VI) and Cr(III) on energy metabolism of heterotrophic Euglena gracilis

糖酵解 生物化学 生物 柠檬酸循环 氧化磷酸化 纤细眼虫 细胞呼吸 柠檬酸合酶 新陈代谢 线粒体 呼吸 谷胱甘肽 乳酸脱氢酶 胞浆 丙酮酸脱氢酶复合物 NAD+激酶 植物 基因 叶绿体
作者
Ricardo Jasso‐Chávez,Angélica Pacheco-Rosales,Elizabeth Lira-Silva,Juan Carlos Gallardo‐Pérez,Noemı́ Garcı́a,Rafael Moreno‐Sánchez
出处
期刊:Aquatic Toxicology [Elsevier]
卷期号:100 (4): 329-338 被引量:33
标识
DOI:10.1016/j.aquatox.2010.08.006
摘要

To assess the toxic effect of Cr on energy metabolism, heterotrophic Euglena gracilis was grown in a medium that prompts high yield biomass and in the presence of different Cr(VI) or Cr(III) concentrations. The cell growth IC50 value was 12 and >250 μM for Cr(VI) and Cr(III), respectively; in these cells chromium was accumulated and a fraction compartmentalized into mitochondria, and synthesis of cysteine and glutathione was induced. Respiration of control isolated mitochondria was strongly inhibited by added Cr(VI) or Cr(III) with L-lactate or succinate as substrates. In turn, cellular and mitochondrial respiration, respiratory Complexes I, III and IV, glycolysis and cytosolic NAD+-alcohol and -lactate dehydrogenases from cells cultured with Cr(VI) were significantly lower than control, whereas AOX and external NADH dehydrogenase activities were unaltered or increased, respectively. Addition of Cr(VI) or Cr(III) to isolated mitochondria or cytosol from control- or Cr(VI)-grown cells induced inhibition of respiration, respiratory Complexes III, IV and AOX, and glycolytic pyruvate kinase; whereas Complex I, external NADH dehydrogenase, and other glycolytic enzymes were unaffected. Protein contents of mitochondrial Complexes I, III, IV and V, and ANT were diminished in Cr(VI)-grown cells. Decreased respiration and glycolysis induced by Cr(VI) resulted in lower cellular ATP content. Results suggested that Cr(VI) cytotoxicity altered gene expression (as widely documented) and hence enzyme content, and induced oxidative stress, but it was also related with direct enzyme inhibition; Cr(III) was also cytotoxic although at higher concentrations. These findings establish new paradigms for chromium toxicity: Cr(VI) direct enzyme inhibition and non-innocuous external Cr(III) toxicity.

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