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禽白血病病毒J亚群与传染性法氏囊病病毒双重感染中ceRNA网络及枢纽基因的综合分析

A Comprehensive Analysis of the ceRNA Network and Hub Genes in Avian Leukosis Virus Subgroup J and Infectious Bursal Disease Virus Superinfection.

作者信息

Chen Sheng, Xu Huijuan, Pan Tingxi, Nie Yu, Zhang Xinheng, Chen Feng, Xie Qingmei, Chen Weiguo

机构信息

State Key Laboratory of Swine and Poultry Breeding Industry & Heyuan Branch, Guangdong Provincial Laboratory of Lingnan Modern Agricultural Science and Technology, College of Animal Science, South China Agricultural University, Guangzhou 510642, China.

Guangdong Provincial Key Lab of AgroAnimal Genomics and Molecular Breeding, College of Animal Science, South China Agricultural University, Guangzhou 510642, China.

出版信息

Animals (Basel). 2024 Nov 28;14(23):3449. doi: 10.3390/ani14233449.

Abstract

In the realm of poultry production, viral superinfections pose significant challenges, causing substantial economic losses worldwide. Among these, avian leukosis virus subgroup J (ALV-J) and infectious bursal disease virus (IBDV) are particularly concerning as they frequently lead to superinfections in chicken, further exacerbating production losses and health complications. Our previous research delved into the pathogenicity and immunosuppressive effects of these superinfections through in vitro and in vivo analyses. Yet, the underlying key genes and pathways governing this phenomenon remained elusive. In this study, we randomly selected three chickens at 21 days post infection from each treatment group (ALV-J, IBDV, ALV-J+IBDV, and control group) to collect the bursa of Fabricius samples for full transcriptome analysis. Utilizing these data, we constructed a comprehensive circRNA/lncRNA-miRNA-mRNA network which elucidated both synergistic and specific activations during the superinfection. Notably, three pivotal genes (FILIP1L, DCX, and MYPN) were pinpointed in datasets reflecting synergistic activations. Conversely, four other genes (STAP, HKR6, XKR4, and TLR5) emerged in datasets associated with specific activations. Further exploration revealed diverse significant GO terms and pathways associated with both synergistic and distinct activation processes. These ceRNA network and core genes potentially wield substantial influence over the synergistic or specific activation of tumorigenesis and pathogenesis induced by ALV-J and IBDV. These findings could help develop targeted therapies and improve disease control in poultry, reducing economic losses.

摘要

在家禽生产领域,病毒混合感染带来了重大挑战,在全球范围内造成了巨大的经济损失。其中,禽J亚群白血病病毒(ALV-J)和传染性法氏囊病病毒(IBDV)尤为令人担忧,因为它们经常导致鸡群发生混合感染,进一步加剧生产损失和健康问题。我们之前的研究通过体外和体内分析,深入探讨了这些混合感染的致病性和免疫抑制作用。然而,控制这一现象的潜在关键基因和途径仍然不清楚。在本研究中,我们从每个处理组(ALV-J、IBDV、ALV-J+IBDV和对照组)中随机选择3只感染后21天的鸡,采集法氏囊样本进行全转录组分析。利用这些数据,我们构建了一个全面的circRNA/lncRNA-miRNA-mRNA网络,该网络阐明了混合感染过程中的协同激活和特异性激活。值得注意的是,在反映协同激活的数据集中确定了三个关键基因(FILIP1L、DCX和MYPN)。相反,在与特异性激活相关的数据集中出现了另外四个基因(STAP、HKR6、XKR4和TLR5)。进一步的探索揭示了与协同激活和独特激活过程相关的各种重要的基因本体论(GO)术语和途径。这些竞争性内源RNA(ceRNA)网络和核心基因可能对ALV-J和IBDV诱导的肿瘤发生和发病机制的协同或特异性激活具有重大影响。这些发现有助于开发针对性的治疗方法,改善家禽疾病控制,减少经济损失。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d26/11640342/d5425efded84/animals-14-03449-g001.jpg

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