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Poliovirus tropism and attenuation are determined after internal ribosome entry
Steven E. Kauder, Vincent R. Racaniello
Steven E. Kauder, Vincent R. Racaniello
Published June 15, 2004
Citation Information: J Clin Invest. 2004;113(12):1743-1753. https://doi.org/10.1172/JCI21323.
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Article Virology

Poliovirus tropism and attenuation are determined after internal ribosome entry

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Abstract

Poliovirus replication is limited to a few organs, including the brain and spinal cord. This restricted tropism may be a consequence of organ-specific differences in translation initiation by the poliovirus internal ribosome entry site (IRES). A C-to-U mutation at base 472 in the IRES of the Sabin type 3 poliovirus vaccine strain, known to attenuate neurovirulence, may further restrict tropism by eliminating viral replication in the CNS. To determine the relationship between IRES-mediated translation and poliovirus tropism, recombinant human adenoviruses were used to express bicistronic mRNAs in murine organs. The IRESs of poliovirus, the cardiotropic coxsackievirus B3 (CVB3), and the hepatotropic hepatitis C virus (HCV) mediate translation in many organs, including those that do not support viral replication. A translation defect associated with the Sabin type 3 IRES was observed in all organs examined. Poliovirus type 1 and recombinant polioviruses dependent on the IRES of CVB3 or HCV replicate in the CNS of mice and cause paralysis. Although the type 3 Sabin strain is an effective vaccine, polioviruses with a U at base 472 of the IRES cause paralysis in newborn mice. Tropism of wild-type and vaccine strains of poliovirus is therefore determined after internal ribosome entry.

Authors

Steven E. Kauder, Vincent R. Racaniello

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Figure 4

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Replication and virulence of recombinant poliovirus strains. (A) Genome ...
Replication and virulence of recombinant poliovirus strains. (A) Genome structure of poliovirus type 1 strain Mahoney, recombinant strain P1/CVB3, and recombinant strain P1/HCV. IRES, predicted AUG initiation codons, and poliovirus polyprotein (open box) are indicated. Translation of P1/HCV is predicted to initiate at the HCV AUG initiation codon, which is followed by 369 nucleotides of HCV polyprotein sequence (lined box). Sequence encoding the recognition site for poliovirus protease 2Apro (triangle) separates HCV sequence and nucleotide 745 of the poliovirus genome. (B) Single-step replication analysis in HeLa cells of poliovirus type 1 strain Mahoney (squares), P1/CVB3 (triangles), and P1/HCV (circles). Data points are the mean of two infections.

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