Utilization of sialic acid as a coreceptor is required for reovirus-induced biliary disease
Erik S. Barton, … , J. Denise Wetzel, Terence S. Dermody
Erik S. Barton, … , J. Denise Wetzel, Terence S. Dermody
Published June 15, 2003
Citation Information: J Clin Invest. 2003;111(12):1823-1833. https://doi.org/10.1172/JCI16303.
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Utilization of sialic acid as a coreceptor is required for reovirus-induced biliary disease

Abstract

Infection of neonatal mice with some reovirus strains produces a disease similar to infantile biliary atresia, but previous attempts to correlate reovirus infection with this disease have yielded conflicting results. We used isogenic reovirus strains T3SA– and T3SA+, which differ solely in the capacity to bind sialic acid as a coreceptor, to define the role of sialic acid in reovirus encephalitis and biliary tract infection in mice. Growth in the intestine was equivalent for both strains following peroral inoculation. However, T3SA+ spread more rapidly from the intestine to distant sites and replicated to higher titers in spleen, liver, and brain. Strikingly, mice infected with T3SA+ but not T3SA– developed steatorrhea and bilirubinemia. Liver tissue from mice infected with T3SA+ demonstrated intense inflammation focused at intrahepatic bile ducts, pathology analogous to that found in biliary atresia in humans, and high levels of T3SA+ antigen in bile duct epithelial cells. T3SA+ bound 100-fold more efficiently than T3SA– to human cholangiocarcinoma cells. These observations suggest that the carbohydrate-binding specificity of a virus can dramatically alter disease in the host and highlight the need for epidemiologic studies focusing on infection by sialic acid–binding reovirus strains as a possible contributor to the pathogenesis of neonatal biliary atresia.

Authors

Erik S. Barton, Bryan E. Youree, Daniel H. Ebert, J. Craig Forrest, Jodi L. Connolly, Tibor Valyi-Nagy, Kay Washington, J. Denise Wetzel, Terence S. Dermody

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Figure 5

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Serum alkaline phosphatase and bilirubin levels in mice after infection ...
Serum alkaline phosphatase and bilirubin levels in mice after infection with T3SA– and T3SA+. ND4 Swiss Webster mice, 2–3 days old, were inoculated perorally with 2.5 × 103 PFU of either T3SA– or T3SA+. Mock-infected animals were inoculated perorally with PBS. At the indicated times after inoculation, mice were euthanized, blood was collected, and serum was separated by centrifugation. Total alkaline phosphatase (a) and bilirubin (b) levels were determined for each serum sample. Each bar represents an average enzyme level for one to four mice. Error bars indicate SEM. *P < 0.05, T3SA– vs. T3SA+ by Student t test.