4.4 Review

Histologic Lesions Induced by Murine Norovirus Infection in Laboratory Mice

Journal

VETERINARY PATHOLOGY
Volume 53, Issue 4, Pages 754-763

Publisher

SAGE PUBLICATIONS INC
DOI: 10.1177/0300985815618439

Keywords

atherosclerosis; Caliciviridae; calicivirus; histopathology; laboratory animals; murine norovirus; pathology; laboratory mice; Stat1SUP-; -; IfnR-; -

Funding

  1. National Institutes of Health [R21-OD011135, R01-OD011149]
  2. University of Washington's Nutrition Obesity Research Center [P30-DK035816]

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Murine noroviruses (MNVs) are highly prevalent in laboratory mice, can cause persistent infections, and have been shown to infect macrophages, dendritic cells, and B cells. To address the potential impact of MNV infection on research outcomes, numerous studies have been conducted with various mouse models of human disease and have generated mixed results, ranging from no impact to significant disease. Many of these studies included histologic evaluations after MNV infection, and these results have similarly been variable in terms of whether MNV induces lesions, despite the fact that localization of MNV by viral culture and molecular techniques have demonstrated systemic distribution regardless of mouse immune status. The aim of this review is to summarize the histologic findings that have been reported with MNV infection in several mouse models. The studies demonstrate that experimental infection of MNV in wild-type mice results in minimal to no histologic changes. In contrast, immunodeficient mice consistently have detectable MNV-induced lesions that are typically inflammatory and, in the most severe cases, accompanied by necrosis. In these, the liver is commonly affected, with more variable lesions reported in the lung, gastrointestinal tract, mesenteric lymph nodes, brain, and spleen. In specific disease models including atherosclerosis, MNV infection had a variable impact that was dependent on the mouse model, viral strain, timing of infection, or other experimental variables. It is important to recognize the reported MNV lesions to help discern the possible influence of MNV infection on data generated in mouse models.

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