Macroautophagy proteins assist epstein barr virus production and get incorporated into the virus particles

Heike Nowag, Bruno Guhl, Kerstin Thriene, Susana Romao, Urs Ziegler, Joern Dengjel, Christian Münz

Research output: Contribution to journalArticlepeer-review

92 Scopus citations

Abstract

Epstein Barr virus (EBV) persists as a latent herpes virus infection in themajority of the adult human population. The virus can reactivate fromthis latent infection into lytic replication for virus particle production. Here, we report that autophagic membranes, which engulf cytoplasmic constituents during macroautophagy and transport them to lysosomal degradation, are stabilized by lytic EBV replication in infected epithelial and B cells. Inhibition of autophagic membrane formation compromises infectious particle production and leads to the accumulation of viral DNA in the cytosol. Vice versa, pharmacological stimulation of autophagic membrane formation enhances infectious virus production. Atg8/LC3, an essential macroautophagy protein and substrate anchor on autophagic membranes, was found in virus preparations, suggesting that EBV recruits Atg8/LC3 coupled membranes to its envelope in the cytosol. Our data indicate that EBV subverts macroautophagy and uses autophagic membranes for efficient envelope acquisition during lytic infection.

Original languageEnglish
Pages (from-to)116-125
Number of pages10
JournaleBioMedicine
Volume1
Issue number2-3
DOIs
StatePublished - 2014
Externally publishedYes

Keywords

  • Atg12
  • Atg16
  • Atg8/Lc3
  • B cell
  • Bzlf1
  • Epithelial cell
  • Lytic Ebv replication

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