| Literature DB >> 21238947 |
Bing-Ching Ho1, Sung-Liang Yu, Jeremy J W Chen, Sui-Yuan Chang, Bo-Shiun Yan, Qi-Sheng Hong, Sher Singh, Chuan-Liang Kao, Hsuan-Yu Chen, Kang-Yi Su, Ker-Chau Li, Chiou-Ling Cheng, Hao-Wei Cheng, Jen-Yi Lee, Chun-Nan Lee, Pan-Chyr Yang.
Abstract
Viruses rely on the host translation machinery to complete their life cycles. Picornaviruses use an internal ribosome entry site to initiate cap-independent protein translation and in parallel host cap-dependent translation is shut off. This process is thought to occur primarily via cleavage of host translation initiation factors eIF4GI and eIF4GII by viral proteases. Here we describe another mechanism whereby miR-141 induced upon enterovirus infection targets the cap-dependent translation initiation factor, eIF4E, for shutoff of host protein synthesis. Knockdown of miR-141 reduces viral propagation, and silencing of eIF4E can completely reverse the inhibitory effect of the miR-141 antagomiR on viral propagation. Ectopic expression of miR-141 promotes the switch from cap-dependent to cap-independent translation. Moreover, we identified a transcription factor, EGR1, which is partly responsible for miR-141 induction in response to enterovirus infection. Our results suggest that upregulation of miR-141 upon enterovirus infection can facilitate viral propagation by expediting the translational switch. Copyright ÂEntities:
Mesh:
Substances:
Year: 2011 PMID: 21238947 DOI: 10.1016/j.chom.2010.12.001
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023