Figure - PMC

Skip to main content

An official website of the United States government

Here's how you know

Here's how you know

Official websites use .gov
A .gov website belongs to an official government organization in the United States.

Secure .gov websites use HTTPS
A lock ( ) or https:// means you've safely connected to the .gov website. Share sensitive information only on official, secure websites.

View full-text article in PMC

. 2020 May 20;117(22):12249–12257. doi: 10.1073/pnas.2006106117

Search in PMC
Search in PubMed
View in NLM Catalog
Add to search

Copyright © 2020 the Author(s). Published by PNAS.

This open access article is distributed under Creative Commons Attribution-NonCommercial-NoDerivatives License 4.0 (CC BY-NC-ND).

PMC Copyright notice

Fig. 4. — Model for viral infection effects on TEs in carcasses. (A) In uninfected conditions, TEs are controlled by piRNAs and siRNAs. (B) Upon infection, the dsRNA uptake pathway allows the systemic spread of viral RNAs, and this machinery also opportunistically carries TE dsRNA intermediates and allows for their spread. This triggers the systemic production of virus-derived siRNAs as well as TE-derived siRNAs, which subsequently leads to the reduction of TE transcript amounts in carcasses. The uptaken TE RNAs are also substrates for piRNA synthesis, which strengthen TE posttranscriptional silencing. (C) In case the siRNA pathway is impaired (e.g., dcr2^−/− mutant, or viral RNAi suppressor targeting Dcr-2), viral replication increases, and we propose that viral RNAs saturate the piRNA pathway, which is no longer available for TEs. This results in an increase in TE transcript amounts.