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首页> 外文期刊>Molecular and Biochemical Parasitology >Proteomic analysis of two populations of Schistosoma mansoni-derived extracellular vesicles: 15k pellet and 120k pellet vesicles
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Proteomic analysis of two populations of Schistosoma mansoni-derived extracellular vesicles: 15k pellet and 120k pellet vesicles

机译:两种血吸虫麦森衍生细胞外囊囊泡蛋白质组学分析:15K颗粒和120K颗粒囊泡

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摘要

Helminth parasites secrete extracellular vesicles (EVs) into their environment that have potential roles in hostparasite communication, and thus represent potentially useful targets for novel control strategies. Here, we carried out a comprehensive proteomic analysis of two different populations of EVs - 15k pellet and 120k pellet EVs - from Schistosoma mansoni adult worms. We characterised the proteins present in the membranes of the EVs (including external trypsin-liberated peptides, integral membrane proteins (IMPs) and peripheral membrane proteins (PMPs)), as well as cargo proteins, using LC-MS/MS. A total of 286 and 716 proteins were identified in 15k and 120k pellets, respectively. Some of the most abundant proteins identified from both 15k and 120k pellets include known vaccine candidates such as Sm-TSP-2, saponin B domain-containing proteins, calpain glutathione-S-transferase, Sm29 and cathepsin domain-containing proteins. Other abundant proteins that have not been tested as vaccines include DM9 domain-containing protein, 13 kDa tegumental antigen and histone H4like protein. Sm23, a member of the tetraspanin family with known vaccine efficacy, was identified in the cargo and IMP compartments of only 15k pellet vesicles. Moreover, a collection of proteins with known or potential relevance in host-parasite communication including proteases, antioxidants and EV biogenesis/trafficking of both vesicle types were identified. Our results provide the first report of a comprehensive compartmental proteomic analysis of adult S. mansoni-derived EVs. Future research should investigate recombinant forms of these proteins as vaccine and serodiagnostic antigens as well as the roles of EV proteins in host-parasite communication.
机译:Helminth Parasites分泌细胞外囊(EVS)进入其环境中具有潜在作用的潜在作用,因此代表了新的控制策略的潜在有用的目标。在这里,我们对来自Schistosoma Mansoni成人蠕虫的两种不同群体的综合蛋白质组学分析了两种不同群体。我们以使用LC-MS / MS的表征在EVS的膜中存在的蛋白质(包括外部胰蛋白酶 - 释放的肽,整体膜蛋白(Imms)和外周膜蛋白(PMP)),以及货物蛋白质。共有286和716个蛋白质分别在15K和120K颗粒中鉴定出来。从15K和120K颗粒中鉴定的一些最丰富的蛋白质包括已知的疫苗候选者,例如SM-TSP-2,含有皂苷B域域,Calpain谷胱甘肽-S-转移酶,SM29和含组织蛋白酶域域的蛋白质。尚未测试为疫苗的其他丰富的蛋白质包括DM9含域的蛋白质,13kDA Tegumental抗原和组蛋白H4样蛋白。 SM23是具有已知疫苗疗效的四胞苷家族的成员,在货物和仅15K颗粒囊泡中的爆屑盒中鉴定出来。此外,鉴定了在包括蛋白酶,抗氧化剂和EV生物发生/运输两种囊泡类型的宿主寄生虫通信中具有已知或潜在相关性的蛋白质的集合。我们的结果提供了成人S. Mansoni衍生EV的综合隔间蛋白质组学分析的第一份报告。未来的研究应调查这些蛋白质的重组形式作为疫苗和血清诊断抗原以及EV蛋白在寄生虫通信中的作用。

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