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29.06.2016 | Original Article

The LXR ligand GW3965 inhibits Newcastle disease virus infection by affecting cholesterol homeostasis

verfasst von: Xiang-xiang Sheng, Ying-jie Sun, Yuan Zhan, Yu-rong Qu, Hua-xia Wang, Miao Luo, Ying Liao, Xu-sheng Qiu, Chan Ding, Hong-jie Fan, Xiang Mao

Erschienen in: Archives of Virology | Ausgabe 9/2016

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Abstract

Newcastle disease (ND) is a contagious disease that affects most species of birds. Its causative pathogen, Newcastle disease virus (NDV), also exhibits considerable oncolytic activity against mammalian cancers. A better understanding of the pathogenesis of NDV will help us design efficient vaccines and novel anticancer strategies. GW3965, a widely used synthetic ligand of liver X receptor (LXR), induces the expression of LXRs and its downstream genes, including ATP-binding cassette transporter A1 (ABCA1). ABCA1 regulates cellular cholesterol homeostasis. Here, we found that GW3965 inhibited NDV infection in DF-1 cells. It also inhibited NF-κB activation and reduced the upregulation of proinflammatory cytokines induced by the infection. Further studies showed that GW3965 exerted its inhibitory effects on virus entry and replication. NDV infection increased the mRNA levels of several lipogenic genes but decreased the ABCA1 mRNA level. Overexpression of ABCA1 inhibited NDV infection and reduced the cholesterol content in DF-1 cells, but when the cholesterol was replenished, NDV infection was restored. GW3965 treatment prevented cholesterol accumulation in the perinuclear area of the infected cells. In summary, our studies suggest that GW3965 inhibits NDV infection, probably by affecting cholesterol homeostasis.

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Titel: The LXR ligand GW3965 inhibits Newcastle disease virus infection by affecting cholesterol homeostasis
verfasst von: Xiang-xiang Sheng
Ying-jie Sun
Yuan Zhan
Yu-rong Qu
Hua-xia Wang
Miao Luo
Ying Liao
Xu-sheng Qiu
Chan Ding
Hong-jie Fan
Xiang Mao
Publikationsdatum: 29.06.2016
Verlag: Springer Vienna
Erschienen in: Archives of Virology / Ausgabe 9/2016
Print ISSN: 0304-8608
Elektronische ISSN: 1432-8798
DOI: https://doi.org/10.1007/s00705-016-2950-4

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