Competing endogenous RNA network profiling reveals novel host dependency factors required for MERS-CoV propagation

Xi Zhang(University of Hong Kong), Hin Chu(University of Hong Kong), Lei Wen(University of Hong Kong), Huiping Shuai(University of Hong Kong), Dong Yang(University of Hong Kong), Yixin Wang(University of Hong Kong), Yuxin Hou(University of Hong Kong), Zheng Zhu(University of Hong Kong), Shuofeng Yuan(University of Hong Kong), Feifei Yin(Hainan Medical University), Jasper Fuk‐Woo Chan(University of Hong Kong - Shenzhen Hospital), Kwok‐Yung Yuen(University of Hong Kong - Shenzhen Hospital)
Emerging Microbes & Infections
January 1, 2020
Cited by 76Open Access
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Abstract

< 0.001) increased at 24 h-post infection. These DE circRNAs were clustered into 4 groups according to their time-course expression patterns and demonstrated inter-cluster and intra-cluster variations in the predicted functions of their host genes. Our comprehensive circRNA-miRNA-mRNA network identified 7 key DE circRNAs involved in various biological processes upon MERS-CoV infection. Specific siRNA knockdown of two selected DE circRNAs (circFNDC3B and circCNOT1) significantly reduced MERS-CoV load and their target mRNA expression which modulates various biological pathways, including the mitogen-activated protein kinase (MAPK) and ubiquitination pathways. These results provided novel insights into the ceRNA network perturbations, biological relevance of circRNAs, and potential host-targeting antiviral strategies for MERS-CoV infection.


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