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Glycerol supports growth of the Trypanosoma brucei bloodstream forms in the absence of glucose: Analysis of metabolic adaptations on glycerol-rich conditions

机译:甘油在缺乏葡萄糖的情况下支持布鲁氏锥虫血流形式的生长:在富含甘油的条件下的代谢适应性分析

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摘要

The bloodstream forms of Trypanosoma brucei (BSF), the parasite protist causing sleeping sickness, primarily proliferate in the blood of their mammalian hosts. The skin and adipose tissues were recently identified as additional major sites for parasite development. Glucose was the only carbon source known to be used by bloodstream trypanosomes to feed their central carbon metabolism, however, the metabolic behaviour of extravascular tissue-adapted parasites has not been addressed yet. Since the production of glycerol is an important primary function of adipocytes, we have adapted BSF trypanosomes to a glucose-depleted but glycerol-rich culture medium (CMM_Glyc/GlcNAc) and compared their metabolism and proteome to those of parasites grown in standard glucose-rich conditions (CMM_Glc). BSF were shown to consume 2-folds more oxygen per consumed carbon unit in CMM_Glyc/GlcNAc and were 11.5-times more sensitive to SHAM, a specific inhibitor of the plant-like alternative oxidase (TAO), which is the only mitochondrial terminal oxidase expressed in BSF. This is consistent with (i) the absolute requirement of the mitochondrial respiratory activity to convert glycerol into dihydroxyacetone phosphate, as deduced from the updated metabolic scheme and (ii) with the 1.8-fold increase of the TAO expression level compared to the presence of glucose. Proton NMR analysis of excreted end products from glycerol and glucose metabolism showed that these two carbon sources are metabolised through the same pathways, although the contributions of the acetate and succinate branches are more important in the presence of glycerol than glucose (10.2% versus 3.4% of the excreted end products, respectively). In addition, metabolomic analyses by mass spectrometry showed that, in the absence of glucose, 13C-labelled glycerol was incorporated into hexose phosphates through gluconeogenesis. As expected, RNAi-mediated down-regulation of glycerol kinase expression abolished glycerol metabolism and was lethal for BSF grown in CMM_Glyc/GlcNAc. Interestingly, BSF have adapted their metabolism to grow in CMM_Glyc/GlcNAc by concomitantly increasing their rate of glycerol consumption and decreasing that of glucose. However, the glycerol kinase activity was 7.8-fold lower in CMM_Glyc/GlcNAc, as confirmed by both western blotting and proteomic analyses. This suggests that the huge excess in glycerol kinase that is not absolutely required for glycerol metabolism, might be used for another yet undetermined non-essential function in glucose rich-conditions. Altogether, these data demonstrate that BSF trypanosomes are well-adapted to glycerol-rich conditions that could be encountered by the parasite in extravascular niches, such as the skin and adipose tissues.
机译:布鲁氏锥虫(BSF)的血液形式,是导致昏睡病的寄生虫生物,主要在其哺乳动物宿主的血液中增殖。皮肤和脂肪组织最近被确定为寄生虫发育的其他主要部位。葡萄糖是已知的唯一一种碳源,可被血锥虫用于补充其中心碳代谢,但是,尚未解决血管外组织适应性寄生虫的代谢行为。由于甘油的产生是脂肪细胞的重要主要功能,因此我们使BSF锥虫适应了葡萄糖缺乏但富含甘油的培养基(CMM_Glyc / GlcNAc),并将它们的代谢和蛋白质组与标准葡萄糖含量高的寄生虫的代谢和蛋白质组进行了比较。条件(CMM_Glc)。在CMM_Glyc / GlcNAc中,每单位碳单位的BSF消耗的氧气多2倍,对SHAM的敏感性高11.5倍,SHAM是植物样替代氧化酶(TAO)的特异性抑制剂,后者是唯一表达的线粒体末端氧化酶在BSF中。这符合(i)从更新的代谢方案推导的线粒体呼吸活动将甘油转化为磷酸二羟基丙酮的绝对要求,以及(ii)与葡萄糖的存在相比,TAO表达水平提高了1.8倍。甘油和葡萄糖代谢过程中排出的终产物的质子NMR分析表明,这两种碳源通过相同的途径代谢,尽管在甘油存在下乙酸根和琥珀酸分支的贡献比葡萄糖更重要(10.2%对3.4%分别排泄的最终产品)。此外,质谱的代谢组学分析表明,在不存在葡萄糖的情况下, 13 C标记的甘油通过糖异生作用被掺入到己糖磷酸中。不出所料,RNAi介导的甘油激酶表达下调消除了甘油代谢,并且对CMM_Glyc / GlcNAc中生长的BSF致死。有趣的是,BSF通过同时增加其甘油的消耗速率和降低其葡萄糖的含量,使其代谢在CMM_Glyc / GlcNAc中生长。然而,如通过蛋白质印迹和蛋白质组学分析所证实,在CMM_Glyc / GlcNAc中,甘油激酶活性降低了7.8倍。这表明甘油代谢并非绝对必需的甘油激酶的巨大过量,可用于在葡萄糖丰富的条件下另一种尚未确定的非必需功能。总而言之,这些数据表明BSF锥虫体非常适合于富含甘油的疾病,这种寄生虫可能在诸如皮肤和脂肪组织等血管外生境中被寄生虫所遇到。

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