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港海豹的大脑转录组显示了患有代谢疾病和病毒感染的动物的基因表达模式。

Brain transcriptomes of harbor seals demonstrate gene expression patterns of animals undergoing a metabolic disease and a viral infection.

作者信息

Rosales Stephanie M, Vega Thurber Rebecca L

机构信息

Department of Microbiology, Oregon State University , Corvallis , OR , United States.

出版信息

PeerJ. 2016 Dec 22;4:e2819. doi: 10.7717/peerj.2819. eCollection 2016.

Abstract

Diseases of marine mammals can be difficult to diagnose because of their life history and protected status. Stranded marine mammals have been a particularly useful resource to discover and comprehend the diseases that plague these top predators. Additionally, advancements in high-throughput sequencing (HTS) has contributed to the discovery of novel pathogens in marine mammals. In this study, we use a combination of HTS and stranded harbor seals () to better understand a known and unknown brain disease. To do this, we used transcriptomics to evaluate brain tissues from seven neonatal harbor seals that expired from an unknown cause of death (UCD) and compared them to four neonatal harbor seals that had confirmed phocine herpesvirus (PhV-1) infections in the brain. Comparing the two disease states we found that UCD animals showed a significant abundance of fatty acid metabolic transcripts in their brain tissue, thus we speculate that a fatty acid metabolic dysregulation contributed to the death of these animals. Furthermore, we were able to describe the response of four young harbor seals with PhV-1 infections in the brain. PhV-1 infected animals showed a significant ability to mount an innate and adaptive immune response, especially to combat viral infections. Our data also suggests that PhV-1 can hijack host pathways for DNA packaging and exocytosis. This is the first study to use transcriptomics in marine mammals to understand host and viral interactions and assess the death of stranded marine mammals with an unknown disease. Furthermore, we show the value of applying transcriptomics on stranded marine mammals for disease characterization.

摘要

由于海洋哺乳动物的生活史和受保护地位,其疾病可能难以诊断。搁浅的海洋哺乳动物一直是发现和理解困扰这些顶级捕食者的疾病的特别有用的资源。此外,高通量测序(HTS)技术的进步有助于在海洋哺乳动物中发现新的病原体。在本研究中,我们结合使用HTS和搁浅的港海豹来更好地了解一种已知和未知的脑部疾病。为此,我们使用转录组学来评估七只因不明死因(UCD)死亡的新生港海豹的脑组织,并将它们与四只脑部确诊感染海豹疱疹病毒(PhV-1)的新生港海豹进行比较。比较这两种疾病状态,我们发现UCD动物的脑组织中脂肪酸代谢转录本显著丰富,因此我们推测脂肪酸代谢失调导致了这些动物的死亡。此外,我们能够描述四只脑部感染PhV-1的幼年港海豹的反应。感染PhV-1的动物表现出显著的产生先天性和适应性免疫反应的能力,尤其是对抗病毒感染。我们的数据还表明,PhV-1可以劫持宿主的DNA包装和胞吐途径。这是第一项在海洋哺乳动物中使用转录组学来了解宿主与病毒相互作用并评估患有未知疾病的搁浅海洋哺乳动物死亡原因的研究。此外,我们展示了将转录组学应用于搁浅海洋哺乳动物进行疾病特征描述的价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c22c/5182994/545ac7365b69/peerj-04-2819-g001.jpg

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