Abstract
BackgroundEnterovirus 71 (EV71 or EV-A71) was first identified in California about half a century ago. In recent years, outbreaks of EV-A71 were prevalent worldwide, including Taiwan, Malaysia, Singapore, Japan, and China. Between 2008 and 2011, China alone reported 1894 deaths associated with EV-A71 infection. In mild cases, EV-A71 can cause herpangina and hand-foot-and-mouth disease (HFMD). However, in severe cases, it could cause neurological disorders, including meningitis and encephalitis. Cardiopulmonary failure is common among hospitalized children with EV-A71 infection. No effective FDA-approved therapeutics against EV-A71 are clinically available.MethodsWe report the establishment of an immunocompetent wild type strain 129 (wt-129) mouse model, which can be cross-species infected with human EV-A71 clinical isolates via an intraperitoneal route.ResultsOne intriguing disease phenotype of this new model is the development of characteristic “White-Jade” patches in the muscle, which lost sporadically the normal pink color of uninfected muscle. Viral VP1 protein and massive leukocyte infiltration were detected in muscles with or without white-jades. We demonstrated further that hypoxia is a general phenomenon associated with white-jades in both immunocompetent and immunodeficient mouse models. Therefore, hypoxia appears to be a feature intrinsic to EV-A71 infection, irrespective of its host’s immunogenetic background. To date, no effective treatment for EV-A71 is available. Here, using this new wt-129 mouse model, we showed that timely treatment with compound R837 (a TLR7 immune modulator) via oral or intraperitoneal routes, rescued the hypoxia, limb paralysis, and death at a high therapeutic efficacy.ConclusionsIn this new immunocompetent mouse 129 model, we observed an unexpected white-jade phenotype and its associated hypoxia. The successful treatment with TLR7 immune modulators via an oral route, provide us a new research direction for EV-A71 basic science and translational research. It remains an open issue whether R837 or its related compounds, will be a promising drug candidate in clinical trials in EV-A71 endemic or epidemic areas in the future.
Highlights
Enterovirus 71 (EV71 or EV-A71) was first identified in California about half a century ago
A new immunocompetent wild type 129 mouse model for EV-A71 infection In EV-A71 infection experiment, one-week-old wt-129 mice were i.p. injected with clinical isolates of EV-A71 at a titer of 107–108 pfu/mouse
We found no apparent changes in the quality or quantity of RBC (Additional file 1: Figure S1d), including the number of red blood cells (RBC count), hemoglobin concentration (HGB value) and hematocrit (HCT value)
Summary
Enterovirus 71 (EV71 or EV-A71) was first identified in California about half a century ago. EV-A71 causes hand-foot-and-mouth disease (HFMD), herpangina and diarrhea in children [1, 2, 7]. Human SCARB2 transgenic mice were shown to be susceptible to EV-A71 infection [19, 20]. These hSCARB2 transgenic mouse models are not without any limitations in research. In the other report [19], the transgenic model is susceptible to a socalled Isehara strain of EV-A71 in Japan. Both transgenic models have very low oral infection efficiency
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