Author:
Shirahama Shintaro,Onoguchi-Mizutani Rena,Kawata Kentaro,Taniue Kenzui,Miki Atsuko,Kato Akihisa,Kawaguchi Yasushi,Tanaka Rie,Kaburaki Toshikatsu,Kawashima Hidetoshi,Urade Yoshihiro,Aihara Makoto,Akimitsu Nobuyoshi
Abstract
Abstract
Long non-coding RNAs (lncRNAs) play vital roles in the pathogenesis of infectious diseases, but the role of lncRNAs in herpes simplex virus 1 (HSV-1) infection remains unknown. Using RNA sequencing analysis, we explored lncRNAs that were highly expressed in murine retinal photoreceptor cell-derived 661W cells infected with HSV-1. U90926 RNA (522 nucleotides) was the most upregulated lncRNA detected post HSV-1 infection. The level of U90926 RNA was continuously increased post HSV-1 infection, reaching a 100-fold increase at 24 h. Cellular fractionation showed that U90926 RNA was located in the nucleus post HSV-1 infection. Downregulation of U90926 expression by RNA interference markedly suppressed HSV-1 DNA replication (80% reduction at 12 h post infection) and HSV-1 proliferation (93% reduction at 12 h post infection) in 661W cells. The survival rates of U90926-knockdown cells were significantly increased compared to those of control cells (81% and 21%, respectively; p < 0.0001). Thus, lncRNA U90926 is crucial for HSV-1 proliferation in retinal photoreceptor cells and consequently leads to host cell death by promoting HSV-1 proliferation.
Funder
Japan Foundation for Applied Enzymology
JSPS KAKENHI
Publisher
Springer Science and Business Media LLC
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