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曼氏血吸虫生命周期中转运凝集素囊泡整合膜蛋白36千道尔顿(VIP36)的分子特征

Molecular characterization of transport lectin vesicular integral membrane protein 36 kDa (VIP36) in the life cycle of Schistosoma mansoni.

作者信息

Ornelas Alice Maria de M, de Paula Renato G, Morais Enyara R, Magalhães Lizandra G, da Silva Annielle M B, Gomes Matheus S, de Castro-Borges William, Rodrigues Vanderlei

机构信息

Department of Genetics, Institute of Biology, Federal University of Rio de Janeiro, Carlos Chagas Filho Av. 373, Rio de Janeiro, Rio de Janeiro, 21941-902, Brazil.

Department of Biochemistry and Immunology, Medicine School of Ribeirão Preto, University of São Paulo, Ribeirão Preto, São Paulo, Brazil.

出版信息

Parasitol Res. 2017 Oct;116(10):2765-2773. doi: 10.1007/s00436-017-5587-7. Epub 2017 Aug 24.

DOI:10.1007/s00436-017-5587-7
PMID:28840376
Abstract

VIP36 is a protein described as an L-type lectin in animals, responsible for the intracellular transport of glycoproteins within the secretory pathway, and also localized on the plasma membrane. Schistosoma mansoni has a complex system of vesicles and protein transport machinery to the cell surface. The excreted/secreted products of the larvae and eggs are known to be exposed to the host immune system. Hence, characterizing the role and action of SmVIP36 in the S. mansoni life cycle is important for a better understanding of the parasite-host relationship. To this purpose, we firstly performed in silico analysis. Analysis of SmVIP36 in silico revealed that it contains a lectin leg-like domain with a jellyroll fold as seen by its putative 3D tertiary structure. Additionally, it was also observed that its CRD contains calcium ion-binding amino acids, suggesting that the binding of SmVIP36 to glycoproteins is calcium-dependent. Finally, we observed that the SmVIP36 predicted amino acid sequence relative to its orthologs was conserved. However, phylogenetic analysis revealed that SmVIP36 follows species evolution, forming a further cluster with its definitive host Homo sapiens. Moreover, q-PCR analysis in the S. mansoni life cycle points to a significant increase in gene expression in the eggs, schistosomulae, and female adult stages. Similarly, protein expression increased in eggs, cercariae, schistosomulae, and adult worm stages. These results suggest that SmVIP36 might participate in the complex secretory activity within the egg envelope and tegument proteins, both important for the stages of the parasite that interact with the host.

摘要

VIP36是一种在动物中被描述为L型凝集素的蛋白质,负责分泌途径中糖蛋白的细胞内运输,并且也定位于质膜上。曼氏血吸虫具有复杂的囊泡系统和蛋白质运输机制以到达细胞表面。已知幼虫和虫卵的排泄/分泌产物会暴露于宿主免疫系统。因此,表征曼氏血吸虫SmVIP36在其生命周期中的作用和作用机制对于更好地理解寄生虫与宿主的关系很重要。为此,我们首先进行了计算机分析。对SmVIP36的计算机分析表明,从其假定的三维三级结构可以看出,它包含一个具有果冻卷折叠的凝集素腿状结构域。此外,还观察到其CRD包含钙离子结合氨基酸,这表明SmVIP36与糖蛋白的结合是钙依赖性的。最后,我们观察到SmVIP36预测的氨基酸序列与其直系同源物相比是保守的。然而,系统发育分析表明,SmVIP36遵循物种进化,与其终末宿主智人形成了一个进一步的聚类。此外,对曼氏血吸虫生命周期的q-PCR分析表明,在虫卵、童虫和雌虫成虫阶段基因表达显著增加。同样,在虫卵、尾蚴、童虫和成虫阶段蛋白质表达也增加。这些结果表明,SmVIP36可能参与了卵包膜和体表蛋白内的复杂分泌活动,这两者对于寄生虫与宿主相互作用的阶段都很重要。

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