Intrinsic antiviral immunity of barrier cells revealed by an iPSC-derived blood-brain barrier cellular model

利用iPSC衍生的血脑屏障细胞模型揭示屏障细胞的内在抗病毒免疫力

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作者:Yichen Cheng ,Angelica Medina ,Zhenlan Yao ,Mausumi Basu ,Janhavi P Natekar ,Jianshe Lang ,Egan Sanchez ,Mezindia B Nkembo ,Chongchong Xu ,Xuyu Qian ,Phuong T T Nguyen ,Zhexing Wen ,Hongjun Song ,Guo-Li Ming ,Mukesh Kumar ,Margo A Brinton ,Melody M H Li ,Hengli Tang

Abstract

Physiological blood-tissue barriers play a critical role in separating the circulation from immune-privileged sites and denying access to blood-borne viruses. The mechanism of virus restriction by these barriers is poorly understood. We utilize induced pluripotent stem cell (iPSC)-derived human brain microvascular endothelial cells (iBMECs) to study virus-blood-brain barrier (BBB) interactions. These iPSC-derived cells faithfully recapitulate a striking difference in in vivo neuroinvasion by two alphavirus isolates and are selectively permissive to neurotropic flaviviruses. A model of cocultured iBMECs and astrocytes exhibits high transendothelial electrical resistance and blocks non-neurotropic flaviviruses from getting across the barrier. We find that iBMECs constitutively express an interferon-induced gene, IFITM1, which preferentially restricts the replication of non-neurotropic flaviviruses. Barrier cells from blood-testis and blood-retinal barriers also constitutively express IFITMs that contribute to the viral resistance. Our application of a renewable human iPSC-based model for studying virus-BBB interactions reveals that intrinsic immunity at the barriers contributes to virus exclusion. Keywords: CP: Immunology; CP: Neuroscience; IFITM; Zika virus; blood-brain barrier; blood-retinal barrier; blood-testis barrier; brain microvascular endothelial cell; dengue virus; flavivirus; intrinsic expression; virus-host interactions.

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