HIF-1alpha-dependent gene expression program during the nucleic acid-triggered antiviral innate immune responses.

Mol Cells

Department of Chemistry and Brain Korea 21 School of Chemical Materials Science, Sungkyunkwan University, Suwon, 440-746, Korea.

Published: February 2009

AI Article Synopsis

  • Recent research indicates that HIF-1alpha has a new role in immune responses, particularly against bacteria and viruses, even in normal oxygen conditions.
  • The study shows that introducing double-stranded nucleic acids, resembling viral genomes, increases HIF-1alpha levels and its target gene expression.
  • This activation of HIF-1alpha is crucial for regulating genes linked to both the hypoxic response and antiviral immune responses, as its reduction leads to less effective immune gene expression.

Article Abstract

Recent studies suggest a novel role of HIF-1alpha under non-hypoxic conditions, including antibacterial and antiviral innate immune responses. However, the identity of the pathogen-associated molecular pattern which triggers HIF-1alpha activation during the antiviral response remains to be identified. Here, we demonstrate that cellular administration of double-stranded nucleic acids, the molecular mimics of viral genomes, results in the induction of HIF-1alpha protein level as well as the increase in HIF-1alpha target gene expression. Whole-genome DNA microarray analysis revealed that double-stranded nucleic acid treatment triggers induction of a number of hypoxia-inducible genes, and induction of these genes are compromised upon siRNA-mediated HIF-1alpha knock-down. Interestingly, HIF-1alpha knock-down also resulted in down-regulation of a number of genes involved in antiviral innate immune responses. Our study demonstrates that HIF-1alpha activation upon nucleic acid-triggered antiviral innate immune responses plays an important role in regulation of genes involved in not only hypoxic response, but also immune response.

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Source
http://dx.doi.org/10.1007/s10059-009-0030-2DOI Listing

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