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The role of mRNA degradation in immunity and inflammation

DOI: 10.1186/ar3562

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Abstract:

We are now focusing on the role of genes induced in response to TLR stimulation, particularly the genes that are rapidly induced in a MyD88-dependent manner within 30 min after LPS stimulation. Among them, we have recently identified a novel gene named Zc3h12a which has a CCCH-type zinc finger domain. The knockout mice developed spontaneous autoimmune diseases accompanied by splenomegaly and lymphadenopathy. Subsequent studies showed that Zc3h12a is a nuclease involved in destabilization of IL-6 and IL-12mRNA. We renamed it Regulatory RNase-1 (Regnase-1) based on the function.We recently found that the IKK complex controls Il6 mRNA stability by phosphorylating Regnase-1 in response to IL-1R/TLR stimulation. Phosphorylated Regnase-1 underwent ubiquitination and degradation. Regnase-1 re-expressed in IL-1R/TLR-activated cells exhibited delayed kinetics, and Regnase-1 mRNA was found to be negatively regulated by Regnase-1 itself via a stem-loop region present in the Regnase-1 3' untranslated region. These data demonstrate that the IKK complex phosphorylates not only IkBalpha, activating transcription, but also Regnase-1, releasing the "brake" on Il6 mRNA expression.

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