Scientific Reports (Jul 2017)

MiR-199a Inhibits Secondary Envelopment of Herpes Simplex Virus-1 Through the Downregulation of Cdc42-specific GTPase Activating Protein Localized in Golgi Apparatus

  • Kyousuke Kobayashi,
  • Fumiko Suemasa,
  • Hiroshi Sagara,
  • Shinya Nakamura,
  • Yasushi Ino,
  • Kazuyoshi Kobayashi,
  • Hiroaki Hiramatsu,
  • Takeshi Haraguchi,
  • Kazuo Kurokawa,
  • Tomoki Todo,
  • Akihiko Nakano,
  • Hideo Iba

DOI
https://doi.org/10.1038/s41598-017-06754-3
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 15

Abstract

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Abstract Because several studies have shown that exogenous miR-199a has antiviral effects against various viruses, including herpesviruses, we examined how miR-199a exerts its antiviral effects using epithelial tumour cell lines infected with herpes simplex virus-1 (HSV-1). We found that both miR-199a-5p and -3p impair the secondary envelopment of HSV-1 by suppressing their common target, ARHGAP21, a Golgi-localized GTPase-activating protein for Cdc42. We further found that the trans-cisternae of the Golgi apparatus are a potential membrane compartment for secondary envelopment. Exogenous expression of either pre-miR-199a or sh-ARHGAP21 exhibited shared phenotypes i.e. alteration of Golgi function in uninfected cells, inhibition of HSV-1 secondary envelopment, and reduction of trans-Golgi proteins upon HSV-1 infection. A constitutively active form of Cdc42 also inhibited HSV-1 secondary envelopment. Endogenous levels of miR-199a in epithelial tumour cell lines were negatively correlated with the efficiency of HSV-1 secondary envelopment within these cells. These results suggest that miR-199a is a crucial regulator of Cdc42 activity on Golgi membranes, which is important for the maintenance of Golgi function and for the secondary envelopment of HSV-1 upon its infection.