Journal of Lipid Research 2014-07-01

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication.

Lukas Bahati Tanner, Charmaine Chng, Xue Li Guan, Zhengdeng Lei, Steven G Rozen, Markus R Wenk

文献索引：J. Lipid Res. 55(7) , 1357-1365, (2014)

摘要

Influenza virus acquires a host-derived lipid envelope during budding, yet a convergent view on the role of host lipid metabolism during infection is lacking. Using a mass spectrometry-based lipidomics approach, we provide a systems-scale perspective on membrane lipid dynamics of infected human lung epithelial cells and purified influenza virions. We reveal enrichment of the minor peroxisome-derived ether-linked phosphatidylcholines relative to bulk ester-linked phosphatidylcholines in virions as a unique pathogenicity-dependent signature for influenza not found in other enveloped viruses. Strikingly, pharmacological and genetic interference with peroxisomal and ether lipid metabolism impaired influenza virus production. Further integration of our lipidomics results with published genomics and proteomics data corroborated altered peroxisomal lipid metabolism as a hallmark of influenza virus infection in vitro and in vivo. Influenza virus may therefore tailor peroxisomal and particularly ether lipid metabolism for efficient replication. Copyright © 2014 by the American Society for Biochemistry and Molecular Biology, Inc.

结构式	名称/CAS号	分子式	全部文献
	D609 钾盐 CAS:83373-60-8	C₁₁H₁₅KOS₂
	2-[[4-[2-[[环己基氨基)羰基](4-环己基丁基)氨基]乙基]苯基]硫基]-2-甲基丙酸 CAS:265129-71-3	C₂₉H₄₆N₂O₃S

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication.

摘要

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