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iTRAQ-Based Quantitative Proteomic Analysis of a Toxigenic Dinoflagellate Alexandrium catenella and Its Non-toxigenic Mutant Exposed to a Cell Cycle Inhibitor Colchicine

机译:基于iTRAQ的毒原性鞭毛藻亚历山大藻链及其非毒突变体暴露于细胞周期抑制剂秋水仙碱的定量蛋白质组学分析

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摘要

Paralytic shellfish toxins (PSTs) are a group of potent neurotoxic alkaloids mainly produced by marine dinoflagellates and their biosynthesis is associated with the cell cycle. Study shows that colchicine can cease cell division and inhibit PST production of dinoflagellates. However, the molecular mechanism behind this linkage is unknown. Here, we applied the iTRAQ-based proteomic approach to investigate protein expression profiles of a toxigenic dinoflagellate Alexandrium catenella (ACHK-T) and its non-toxigenic mutant (ACHK-NT) when treated with colchicine. The results showed that the cell cycles of both strains were arrested at the G1 phase by colchicine, and the toxin biosynthesis of ACHK-T was inhibited. Among 6,988 proteins identified, 113 and 253 proteins were differentially expressed in the colchicine-treated ACHK-T and ACHK-NT, respectively, compared with their non-colchicine treatments. Proteins involved in reactive oxygen species scavenging and protein degradation were upregulated in both strains while proteins participating in photosynthetic pigment biosynthesis and nitrogen metabolism presented different expressions. Nitrate reductase and glutamine synthetase were altered insignificantly in the colchicine-treated ACHK-T while both of them were remarkably downregulated in the colchicine-treated ACHK-NT, suggesting a feedback regulation between PST production and nitrogen metabolism in ACHK-T. Nitrogen originally for PST biosynthesis might be reallocated to photosynthetic pigment biosynthesis in the colchicine-treated ACHK-T. A total of 55 homologs of 7 toxin-related proteins were obtained; however, they altered insignificantly in both colchicine-treated strains, suggesting that toxin biosynthesis might be post-translationally regulated. Our study provided new insights into toxin biosynthesis in marine dinoflagellates.
机译:麻痹性贝类毒素(PSTs)是一组主要由海洋鞭毛藻产生的有效神经毒性生物碱,其生物合成与细胞周期有关。研究表明秋水仙碱可以停止细胞分裂并抑制PNO产生鞭毛。但是,这种联系背后的分子机制尚不清楚。在这里,我们应用基于iTRAQ的蛋白质组学方法研究了秋水仙碱处理后的产毒素性鞭毛亚历山德里亚链霉菌(ACHK-T)及其非产毒突变体(ACHK-NT)的蛋白质表达谱。结果表明秋水仙碱将两种菌株的细胞周期都阻滞在G1期,并抑制了ACHK-T的毒素生物合成。与非秋水仙碱处理相比,在秋水仙碱处理过的ACHK-T和ACHK-NT中鉴定出的6,988个蛋白质中,分别差异表达了113和253个蛋白质。在两种菌株中,参与活性氧清除和蛋白质降解的蛋白质均上调,而参与光合色素生物合成和氮代谢的蛋白质则表达不同。秋水仙碱处理过的ACHK-T中硝酸还原酶和谷氨酰胺合成酶的变化不显着,而秋水仙碱处理过的ACHK-NT中两者均显着下调,表明ACHK-T中PST产生与氮代谢之间存在反馈调节。原本用于PST生物合成的氮可能会在秋水仙碱处理过的ACHK-T中重新分配给光合作用色素生物合成。总共获得了7种毒素相关蛋白的55个同源物。然而,它们在两种秋水仙碱处理过的菌株中变化不大,表明毒素的生物合成可能在翻译后受到调控。我们的研究为海洋鞭毛藻中毒素生物合成提供了新的见识。

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