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成虫并殖吸虫排泄/分泌产物的比较蛋白质组学研究,这些产物是在体外释放的或存在于肺包虫囊肿结节中。

Comparative proteomics of adult Paragonimus kellicotti excretion/secretion products released in vitro or present in the lung cyst nodule.

机构信息

Division of Infectious Diseases, Department of Medicine, Washington University School of Medicine, St. Louis, Missouri, United States of America.

Division of Endocrinology, Metabolism and Lipid Research, Department of Medicine, Washington University School of Medicine, St. Louis, Missouri, United States of America.

出版信息

PLoS Negl Trop Dis. 2022 Aug 17;16(8):e0010679. doi: 10.1371/journal.pntd.0010679. eCollection 2022 Aug.

Abstract

Paragonimus kellicotti is a zoonotic lung fluke infection, the agent of North American paragonimiasis, and an excellent model for other Paragonimus infections. The excretory/secretory proteins (ESP) released by parasites and presented at the parasite-host interface are frequently proposed to be useful targets for drugs and/or vaccines In vitro culture conditions may alter ESP compared to those produced in vivo. In order to investigate ESPs produced in vivo we took advantage of the fact that adult P. kellicotti reproduce in the lungs of experimentally infected gerbils in tissue cysts. We performed a mass-spectrometric analysis of adult P. kellicotti soluble somatic protein (SSPs) extracts, excreted/secreted proteins (ESPs) produced by adult worms during in vitro culture, and lung cyst fluid proteins (CFPs) from experimentally infected gerbils. We identified 2,137 P. kellicotti proteins that were present in at least two of three biological replicates and supported by at least two peptides. Among those were 1,914 proteins found in SSP, 947 in ESP and 37 in CFP. In silico analysis predicted that only 141 of the total 2,137 proteins were secreted via classical or non-classical pathways. The most abundant functional categories in SSP were storage and oxidative metabolism. The most abundant categories in ESP were proteins related to metabolism and signal transduction. The 37 parasite-related proteins in CFP belonged to 11 functional categories. The largest groups were proteins with unknown function, cytoskeletal proteins and proteasome machinery. 29 of these 37 proteins were shared among all three sample types. To our knowledge, this is the first study that compares in vitro and in vivo ESP for any Paragonimus species. This study has provided new insights into ESPs of food-borne trematodes that are produced and released in vivo. Proteins released at the host-parasite interface may help the parasite evade host immunity and may represent new targets for novel treatments or diagnostic tests for paragonimiasis.

摘要

卡拉巴肺吸虫是一种人畜共患的肺部吸虫感染,是北美并殖吸虫病的病原体,也是其他并殖吸虫感染的优秀模型。寄生虫释放的排泄/分泌蛋白(ESP)和寄生虫-宿主界面呈现的蛋白常被提议作为药物和/或疫苗的有用靶点。体外培养条件可能会改变与体内产生的 ESP 相比的 ESP。为了研究体内产生的 ESP,我们利用了这样一个事实,即成年卡拉巴肺吸虫在实验感染沙鼠的肺部组织囊中繁殖。我们对成年卡拉巴肺吸虫可溶性体细胞蛋白(SSP)提取物、成虫在体外培养过程中产生的排泄/分泌蛋白(ESP)以及实验感染沙鼠的肺囊液蛋白(CFP)进行了质谱分析。我们鉴定了 2137 种卡拉巴肺吸虫蛋白,这些蛋白至少在三个生物学重复中的两个中存在,并且至少有两个肽支持。其中,1914 种蛋白存在于 SSP 中,947 种蛋白存在于 ESP 中,37 种蛋白存在于 CFP 中。计算机分析预测,在总共 2137 种蛋白中,只有 141 种是通过经典或非经典途径分泌的。SSP 中最丰富的功能类别是储存和氧化代谢。ESP 中最丰富的类别是与代谢和信号转导相关的蛋白质。CFP 中 37 种寄生虫相关蛋白属于 11 个功能类别。最大的组是具有未知功能的蛋白质、细胞骨架蛋白和蛋白酶体机械。这 37 种蛋白中有 29 种存在于所有三种样本类型中。据我们所知,这是首次比较任何并殖吸虫属物种的体外和体内 ESP 的研究。这项研究为食源性吸虫在体内产生和释放的 ESP 提供了新的见解。寄生虫与宿主相互作用时释放的蛋白可能有助于寄生虫逃避宿主免疫,也可能成为治疗或诊断并殖吸虫病的新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e3e/9423667/b2d4995fc4ae/pntd.0010679.g001.jpg

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