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寄生虫蠕虫 TIMPs 的高通量测序数据集的大规模分析。

TIMPs of parasitic helminths - a large-scale analysis of high-throughput sequence datasets.

机构信息

Center for Biodiscovery and Molecular Development of Therapeutics, Queensland Tropical Health Alliance, James Cook University, Cairns, Queensland, Australia.

出版信息

Parasit Vectors. 2013 May 30;6:156. doi: 10.1186/1756-3305-6-156.

Abstract

BACKGROUND

Tissue inhibitors of metalloproteases (TIMPs) are a multifunctional family of proteins that orchestrate extracellular matrix turnover, tissue remodelling and other cellular processes. In parasitic helminths, such as hookworms, TIMPs have been proposed to play key roles in the host-parasite interplay, including invasion of and establishment in the vertebrate animal hosts. Currently, knowledge of helminth TIMPs is limited to a small number of studies on canine hookworms, whereas no information is available on the occurrence of TIMPs in other parasitic helminths causing neglected diseases.

METHODS

In the present study, we conducted a large-scale investigation of TIMP proteins of a range of neglected human parasites including the hookworm Necator americanus, the roundworm Ascaris suum, the liver flukes Clonorchis sinensis and Opisthorchis viverrini, as well as the schistosome blood flukes. This entailed mining available transcriptomic and/or genomic sequence datasets for the presence of homologues of known TIMPs, predicting secondary structures of defined protein sequences, systematic phylogenetic analyses and assessment of differential expression of genes encoding putative TIMPs in the developmental stages of A. suum, N. americanus and Schistosoma haematobium which infect the mammalian hosts.

RESULTS

A total of 15 protein sequences with high homology to known eukaryotic TIMPs were predicted from the complement of sequence data available for parasitic helminths and subjected to in-depth bioinformatic analyses.

CONCLUSIONS

Supported by the availability of gene manipulation technologies such as RNA interference and/or transgenesis, this work provides a basis for future functional explorations of helminth TIMPs and, in particular, of their role/s in fundamental biological pathways linked to long-term establishment in the vertebrate hosts, with a view towards the development of novel approaches for the control of neglected helminthiases.

摘要

背景

金属蛋白酶组织抑制剂(TIMPs)是一个多功能蛋白家族,它们协调细胞外基质的转化、组织重塑和其他细胞过程。在寄生性蠕虫中,如钩虫,TIMP 被认为在宿主-寄生虫相互作用中发挥关键作用,包括对脊椎动物宿主的入侵和定植。目前,对蠕虫 TIMP 的了解仅限于少数关于犬钩虫的研究,而对于其他引起被忽视疾病的寄生性蠕虫中 TIMP 的发生情况则没有信息。

方法

在本研究中,我们对一系列被忽视的人类寄生虫的 TIMP 蛋白进行了大规模调查,包括美洲钩虫 Necator americanus、蛔虫 Ascaris suum、肝吸虫 Clonorchis sinensis 和华支睾吸虫 Opisthorchis viverrini ,以及血吸虫血吸虫。这需要挖掘现有的转录组和/或基因组序列数据集,以确定已知 TIMP 同源物的存在,预测定义蛋白质序列的二级结构,进行系统的系统发育分析,并评估编码 A. suum、N. americanus 和 Schistosoma haematobium 发育阶段的假定 TIMP 基因的差异表达,这些寄生虫感染哺乳动物宿主。

结果

从寄生虫可用的序列数据集中预测了总共 15 种与已知真核 TIMP 具有高同源性的蛋白质序列,并对其进行了深入的生物信息学分析。

结论

在 RNA 干扰和/或转基因等基因操作技术的可用性的支持下,这项工作为未来对蠕虫 TIMP 的功能探索提供了基础,特别是它们在与脊椎动物宿主长期定植相关的基本生物学途径中的作用/功能,以期为控制被忽视的蠕虫病开发新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/91a5/3679795/30e77f499472/1756-3305-6-156-1.jpg

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