4.6 Article

Stable Formation of Compositionally Unique Stress Granules in Virus-Infected Cells

Journal

JOURNAL OF VIROLOGY
Volume 84, Issue 7, Pages 3654-3665

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/JVI.01320-09

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Funding

  1. Jane Coffin Childs Memorial Fund
  2. NIH [AI064432]
  3. American Cancer Society [RSG109705]
  4. NCRR [P20 RR15587, P20 RR016454]

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Stress granules are sites of mRNA storage formed in response to a variety of stresses, including viral infections. Here, the mechanisms and consequences of stress granule formation during poliovirus infection were examined. The results indicate that stress granules containing T-cell-restricted intracellular antigen 1 (TIA-1) and mRNA are stably constituted in infected cells despite lacking intact RasGAP SH3-domain binding protein 1 (G3BP) and eukaryotic initiation factor 4G. Fluorescent in situ hybridization revealed that stress granules in infected cells do not contain significant amounts of viral positive-strand RNA. Infection does not prevent stress granule formation in response to heat shock, indicating that poliovirus does not block de novo stress granule formation. A mutant TIA-1 protein that prevents stress granule formation during oxidative stress also prevents formation in infected cells. However, stress granule formation during infection is more dependent upon ongoing transcription than is formation during oxidative stress or heat shock. Furthermore, Sam68 is recruited to stress granules in infected cells but not to stress granules formed in response to oxidative stress or heat shock. These results demonstrate that stress granule formation in poliovirus-infected cells utilizes a transcription-dependent pathway that results in the appearance of stable, compositionally unique stress granules.

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