Interferon-Inducible p200-Family Proteins as Novel Sensors of Cytoplasmic DNA: Role in Inflammation and Autoimmunity

書誌事項

公開日
2010-06
権利情報
  • https://journals.sagepub.com/page/policies/text-and-data-mining-license
DOI
  • 10.1089/jir.2009.0096
公開者
SAGE Publications

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説明

<jats:p> Deregulated innate immune responses that result in increased levels of type I interferons (IFNs) and stimulation of IFN-inducible genes are thought to contribute to chronic inflammation and autoimmunity. One family of IFN-inducible genes is the <jats:italic toggle="yes">Ifi200</jats:italic> family, which includes the murine (eg, <jats:italic toggle="yes">Ifi202a, Ifi202b, Ifi203, Ifi204, Mndal</jats:italic> , and <jats:italic toggle="yes">Aim2</jats:italic> ) and human (eg, <jats:italic toggle="yes">IFI16, MNDA, IFIX</jats:italic> , and <jats:italic toggle="yes">AIM2</jats:italic> ) genes. Genes in the family encode structurally related proteins (the p200-family proteins), which share at least one partially conserved repeat of 200-amino acid (200-AA) residues. Consistent with the presence of 2 consecutive oligonucleotide/oligosaccharide-binding folds in the repeat, the p200-family proteins can bind to DNA. Additionally, these proteins (except the p202 proteins) also contain a pyrin (PYD) domain in the N-terminus. Increased expression of p202 proteins in certain strains of female mice is associated with lupus-like disease. Interestingly, only the Aim2 protein is conserved between the mouse and humans. Several recent studies have provided evidence that the Aim2 and p202 proteins can recognize DNA in cytoplasm and the Aim2 protein upon sensing DNA can form a caspase-1-activating inflammasome. In this review, we discuss how the ability of p200-family proteins to sense cytoplasmic DNA may contribute to the development of chronic inflammation and associated diseases. </jats:p>

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