Virus-induced type I IFN stimulates generation of immunoproteasomes at the site of infection
Eui-Cheol Shin, Ulrike Seifert, Takanobu Kato, Charles M. Rice, Stephen M. Feinstone, Peter-M. Kloetzel, Barbara Rehermann
Eui-Cheol Shin, Ulrike Seifert, Takanobu Kato, Charles M. Rice, Stephen M. Feinstone, Peter-M. Kloetzel, Barbara Rehermann
View: Text | PDF
Research Article Immunology

Virus-induced type I IFN stimulates generation of immunoproteasomes at the site of infection

Abstract

IFN-γ is known as the initial and primary inducer of immunoproteasomes during viral infections. We now report that type I IFN induced the transcription and translation of immunoproteasome subunits, their incorporation into the proteasome complex, and the generation of an immunoproteasome-dependent CD8 T cell epitope in vitro and provide in vivo evidence that this mechanism occurs prior to IFN-γ responses at the site of viral infection. Type I IFN–mediated generation of immunoproteasomes was initiated by either poly(I:C) or HCV RNA in human hepatoma cells and was inhibited by neutralization of type I IFN. In serial liver biopsies of chimpanzees with acute HCV infection, increases in immunoproteasome subunit mRNA preceded intrahepatic IFN-γ responses by several weeks, instead coinciding with intrahepatic type I IFN responses. Thus, viral RNA–induced innate immune responses regulate the antigen-processing machinery, which occurs prior to the detection of IFN-γ at the site of infection. This mechanism may contribute to the high effectiveness (95%) of type I IFN–based therapies if administered early during HCV infection.

Authors

Eui-Cheol Shin, Ulrike Seifert, Takanobu Kato, Charles M. Rice, Stephen M. Feinstone, Peter-M. Kloetzel, Barbara Rehermann

×

Figure 5

Immunoproteasome subunit mRNA levels increase early in acute HCV infection and in temporal relation to type I IFN responses.

Options: View larger image (or click on image) Download as PowerPoint
Induction of immunoproteasome subunits in the liver precedes infiltratio...
Five chimpanzees (Ch6455, Ch6461, Ch1606, Ch6475, and Ch6411) were studied prospectively during acute HCV infection. (A) Serum ALT levels (open squares) and serum HCV RNA titers (black diamonds) have previously been reported (44) and are presented for reference purposes. (BG) Serial liver biopsies were analyzed for mRNA levels of (B) β1i (squares) and β7 (triangles); (C) β5i (squares) and β2i (triangles); (D) IFN-γ (squares) and CXCL9 (triangles); (E) TNF-α; (F) 2,5-OAS-1; and (G) IFN-α2 (black line), IFN-α14 (dashed line), IFN-α21 dotted line), and IFN-β (gray line). mRNA levels were normalized to endogenous references (GAPDH and β-actin) and expressed as fold increase over preinfection levels. In Ch1606, the relative mRNA level of IFN-α21 was 36.9 at week 4. Vertical dashed lines separate the time intervals prior to the first major (greater than 2-fold) increase of IFN-γ or TNF-α mRNA levels. NT, not tested due to the shortage of cDNA.