Author: Lai, Mingâ€Chih; Sun, H. Sunny; Wang, Shainnâ€Wei; Tarn, Woanâ€Yuh
Title: DDX3 functions in antiviral innate immunity through translational control of PACT Cord-id: ploi4wh2 Document date: 2015_10_31
ID: ploi4wh2
Snippet: It has emerged that DDX3 plays a role in antiviral innate immunity. However, the exact mechanism by which DDX3 functions in antiviral innate immunity remains to be determined. We found that the expression of the protein activator of the interferonâ€induced protein kinase (PACT) was regulated by DDX3 in human cells. PACT acts as a cellular activator of retinoic acidâ€inducible geneâ€Iâ€like receptors in the sensing of viral RNAs. DDX3 facilitated the translation of PACT mRNA that may contain
Document: It has emerged that DDX3 plays a role in antiviral innate immunity. However, the exact mechanism by which DDX3 functions in antiviral innate immunity remains to be determined. We found that the expression of the protein activator of the interferonâ€induced protein kinase (PACT) was regulated by DDX3 in human cells. PACT acts as a cellular activator of retinoic acidâ€inducible geneâ€Iâ€like receptors in the sensing of viral RNAs. DDX3 facilitated the translation of PACT mRNA that may contain a structured 5′ UTR. Knockdown of DDX3 decreased the viral RNA detection sensitivity of the cells. PACT partially rescued defects of interferonâ€Î²1 and chemokine (Câ€C motif) ligand 5/RANTES (regulated on activation normal T cell expressed and secreted) induction in DDX3â€knockdown HEK293 cells. Therefore, DDX3 may participate in antiviral innate immunity, at least in part, by translational control of PACT. Moreover, we show that overexpression of the hepatitis C virus (HCV) core protein inhibited the translation of a reporter mRNA harboring the PACT 5′ UTR. The HCV core protein was associated and colocalized with DDX3 in cytoplasmic stress granules, suggesting that the HCV core may abrogate the function of DDX3 by sequestering DDX3 in stress granules. The perturbation of DDX3 by viral proteins delineates a critical role for DDX3 in antiviral host defense.
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