The leader proteinase of foot-and-mouth disease virus reduces the immediate-early induction of IFN-beta mRNA and IFN-stimulated gene products, antagonizing the cellular innate immune response.
The leader proteinase of FMDV antagonizes the cellular innate immune response by controlling the transcription of genes involved in innate immunity, including IFN-beta and PKR.
We have previously shown that the leader proteinase (L(pro)) of foot-and-mouth disease virus (FMDV) blocks cap-dependent mRNA translation and that a genetically engineered FMDV lacking the leader proteinase coding region (A12-LLV2) is attenuated in cell culture and susceptible animals. The attenuated phenotype apparently is a consequence of the inability of A12-LLV2 to block the expression of type I interferon (IFN-alpha/beta) protein, resulting in IFN-induced inhibition of FMDV replication. Here we show that in addition to preventing IFN-alpha/beta protein synthesis, L(pro) reduces the level of immediate-early induction of IFN-beta mRNA and IFN-stimulated gene products such as double-stranded RNA-dependent protein kinase R (PKR), 2',5'-oligoadenylate synthetase, and Mx1 mRNAs in swine cells. Down-regulation of cellular PKR by RNA interference did not affect wild-type virus yield but resulted in a higher yield of A12-LLV2, indicating a direct role of PKR in controlling FMDV replication in the natural host. The observation that L(pro) controls the transcription of genes involved in innate immunity reveals a novel role of this protein in antagonizing the cellular response to viral infection.
Santos et al. (Thu,) conducted a other in Foot-and-Mouth Disease Virus infection. Leader proteinase (L(pro)) of FMDV vs. FMDV lacking the leader proteinase coding region (A12-LLV2) was evaluated on Induction of IFN-beta mRNA and IFN-stimulated gene products. The leader proteinase of foot-and-mouth disease virus reduces the immediate-early induction of IFN-beta mRNA and IFN-stimulated gene products, antagonizing the cellular innate immune response.
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