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Schistosome Feeding and Regurgitation

机译:血吸虫喂养和反流

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摘要

Schistosomes are parasitic flatworms that infect >200 million people worldwide, causing the chronic, debilitating disease schistosomiasis. Unusual among parasitic helminths, the long-lived adult worms, continuously bathed in blood, take up nutrients directly across the body surface and also by ingestion of blood into the gut. Recent proteomic analyses of the body surface revealed the presence of hydrolytic enzymes, solute, and ion transporters, thus emphasising its metabolic credentials. Furthermore, definition of the molecular mechanisms for the uptake of selected metabolites (glucose, certain amino acids, and water) establishes it as a vital site of nutrient acquisition. Nevertheless, the amount of blood ingested into the gut per day is considerable: for males ∼100 nl; for the more actively feeding females ∼900 nl, >4 times body volume. Ingested erythrocytes are lysed as they pass through the specialized esophagus, while leucocytes become tethered and disabled there. Proteomics and transcriptomics have revealed, in addition to gut proteases, an amino acid transporter in gut tissue and other hydrolases, ion, and lipid transporters in the lumen, implicating the gut as the site for acquisition of essential lipids and inorganic ions. The surface is the principal entry route for glucose, whereas the gut dominates amino acid acquisition, especially in females. Heme, a potentially toxic hemoglobin degradation product, accumulates in the gut and, since schistosomes lack an anus, must be expelled by the poorly understood process of regurgitation. Here we place the new observations on the proteome of body surface and gut, and the entry of different nutrient classes into schistosomes, into the context of older studies on worm composition and metabolism. We suggest that the balance between surface and gut in nutrition is determined by the constraints of solute diffusion imposed by differences in male and female worm morphology. Our conclusions have major implications for worm survival under immunological or pharmacological pressure.
机译:血吸虫是寄生性扁虫,感染了全世界2亿多人,导致了慢性,使人衰弱的血吸虫病。长寿的成年蠕虫在寄生虫蠕虫中不寻常,它们不断浸入血液中,直接在体表吸收营养,也通过将血液吸收到肠道吸收营养。最近对身体表面进行的蛋白质组学分析表明存在水解酶,溶质和离子转运蛋白,从而强调了其代谢能力。此外,对吸收选定代谢物(葡萄糖,某些氨基酸和水)的分子机制的定义将其确定为营养获取的重要场所。然而,每天摄入肠道的血液量是可观的:雄性约100 nl;雄性约100 nl。对于更积极喂养的雌性动物而言,约为900 nl,> 4倍于身体体积。摄入的红细胞通过专门的食道时会被溶解,而白细胞会被束缚并在那里失去功能。蛋白质组学和转录组学研究表明,除了肠道蛋白酶外,肠道组织中的氨基酸转运蛋白和内腔中的其他水解酶,离子和脂质转运蛋白也暗示了肠道是获取必需脂质和无机离子的场所。表面是葡萄糖的主要进入途径,而肠道则主要是氨基酸的获取,特别是在女性中。血红素是一种潜在毒性的血红蛋白降解产物,会在肠道中积聚,由于血吸虫缺乏肛门,因此必须通过对反流了解不足才能将其排出。在这里,我们将新的观察结果放在体表和肠道的蛋白质组上,并将不同的营养类别输入血吸虫,并纳入有关蠕虫成分和代谢的较早研究的背景中。我们建议,营养表面和肠道之间的平衡取决于雄性和雌性蠕虫形态差异对溶质扩散的限制。我们的结论对蠕虫在免疫或药理学压力下的存活具有重要意义。

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