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比较转录组学和宿主特异性寄生虫基因表达谱为增生性肾病的驱动因素提供了信息。

Comparative transcriptomics and host-specific parasite gene expression profiles inform on drivers of proliferative kidney disease.

机构信息

Scottish Fish Immunology Research Centre, University of Aberdeen, Aberdeen, AB24 2TZ, UK.

Centre for Genome Enabled Biology and Medicine, University of Aberdeen, Aberdeen, AB24 2TZ, UK.

出版信息

Sci Rep. 2021 Jan 25;11(1):2149. doi: 10.1038/s41598-020-77881-7.

Abstract

The myxozoan parasite, Tetracapsuloides bryosalmonae has a two-host life cycle alternating between freshwater bryozoans and salmonid fish. Infected fish can develop Proliferative Kidney Disease, characterised by a gross lymphoid-driven kidney pathology in wild and farmed salmonids. To facilitate an in-depth understanding of T. bryosalmonae-host interactions, we have used a two-host parasite transcriptome sequencing approach in generating two parasite transcriptome assemblies; the first derived from parasite spore sacs isolated from infected bryozoans and the second from infected fish kidney tissues. This approach was adopted to minimize host contamination in the absence of a complete T. bryosalmonae genome. Parasite contigs common to both infected hosts (the intersect transcriptome; 7362 contigs) were typically AT-rich (60-75% AT). 5432 contigs within the intersect were annotated. 1930 unannotated contigs encoded for unknown transcripts. We have focused on transcripts encoding proteins involved in; nutrient acquisition, host-parasite interactions, development, cell-to-cell communication and proteins of unknown function, establishing their potential importance in each host by RT-qPCR. Host-specific expression profiles were evident, particularly in transcripts encoding proteases and proteins involved in lipid metabolism, cell adhesion, and development. We confirm for the first time the presence of homeobox proteins and a frizzled homologue in myxozoan parasites. The novel insights into myxozoan biology that this study reveals will help to focus research in developing future disease control strategies.

摘要

粘孢子虫寄生虫 Tetracapsuloides bryosalmonae 具有二宿主生活史,在淡水苔藓动物和鲑鱼科鱼类之间交替。受感染的鱼类可能会发展出增殖性肾病,其特征是野生和养殖鲑鱼的淋巴样组织驱动的肾脏病理学。为了深入了解 T. bryosalmonae-宿主相互作用,我们使用了二宿主寄生虫转录组测序方法来生成两个寄生虫转录组组装;第一个源自从感染的苔藓动物中分离出的寄生虫孢子囊,第二个源自感染的鱼类肾脏组织。这种方法被采用是为了在没有完整的 T. bryosalmonae 基因组的情况下最小化宿主污染。常见于两种受感染宿主的寄生虫基因(交集转录组;7362 个基因)通常富含 AT(60-75% AT)。交集内的 5432 个基因被注释。1930 个未注释的基因编码未知转录本。我们专注于编码参与;营养获取、宿主-寄生虫相互作用、发育、细胞间通讯和未知功能蛋白的蛋白质的转录本,通过 RT-qPCR 确定它们在每个宿主中的潜在重要性。宿主特异性表达谱明显,特别是在编码蛋白酶和参与脂质代谢、细胞黏附以及发育的蛋白质的转录本中。我们首次证实了粘孢子虫寄生虫中同源盒蛋白和 frizzled 同源物的存在。本研究揭示的粘孢子虫生物学的新见解将有助于集中研究开发未来的疾病控制策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6260/7835236/a66446453b01/41598_2020_77881_Fig1_HTML.jpg

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