Primary infection with dengue or Zika virus does not affect the severity of heterologous secondary infection in macaques.

Meghan E Breitbach,Hansi Dean,Keisuke Yamamoto,Phoenix M Shepherd,Laurel M Stewart,Andrea M Weiler,Jorge E Osorio,Nancy Schultz-Darken,Thomas C Friedrich,Jens Eichkoff,Sallie R Permar,Emma L Mohr,Saverio Capuano,Chelsea M Crooks,Holly Heimsath,Matthew T Aliota,Matthew R Semler,Christina M Newman,David H O’Connor,Dawn M Dudley,Wendy Newton,Ginger Young,Michelle R Koenig,Eric J Peterson ,Gabrielle L Barry

doi:10.1371/journal.ppat.1007766

Meghan E Breitbach, Hansi Dean + Show 23 more

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https://doi.org/10.1371/journal.ppat.1007766

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Abstract

Zika virus (ZIKV) and dengue virus (DENV) are genetically and antigenically related flaviviruses that now co-circulate in much of the tropical and subtropical world. The rapid emergence of ZIKV in the Americas in 2015 and 2016, and its recent associations with Guillain-Barré syndrome, birth defects, and fetal loss have led to the hypothesis that DENV infection induces cross-reactive antibodies that influence the severity of secondary ZIKV infections. It has also been proposed that pre-existing ZIKV immunity could affect DENV pathogenesis. We examined outcomes of secondary ZIKV infections in three rhesus and fifteen cynomolgus macaques, as well as secondary DENV-2 infections in three additional rhesus macaques up to a year post-primary ZIKV infection. Although cross-binding antibodies were detected prior to secondary infection for all animals and cross-neutralizing antibodies were detected for some animals, previous DENV or ZIKV infection had no apparent effect on the clinical course of heterotypic secondary infections in these animals. All animals had asymptomatic infections and, when compared to controls, did not have significantly perturbed hematological parameters. Rhesus macaques infected with DENV-2 approximately one year after primary ZIKV infection had higher vRNA loads in plasma when compared with serum vRNA loads from ZIKV-naive animals infected with DENV-2, but a differential effect of sample type could not be ruled out. In cynomolgus macaques, the serotype of primary DENV infection did not affect the outcome of secondary ZIKV infection.

Highlights

The spread of Zika virus (ZIKV) from Africa to Asia and the Americas has led to the co-circulation and co-infection of ZIKV with other endemic arboviruses including dengue virus (DENV) [1,2,3,4]
We examined secondary ZIKV or DENV infections in rhesus and cynomolgus macaques that had previously been infected with the other virus
We assessed the outcomes of secondary ZIKV or DENV infections by quantifying viral RNA (vRNA) loads, clinical and laboratory parameters, body temperature, and weight for each cohort of animals and compared them with control animals

Summary

Introduction

The spread of Zika virus (ZIKV) from Africa to Asia and the Americas has led to the co-circulation and co-infection of ZIKV with other endemic arboviruses including dengue virus (DENV) [1,2,3,4]. Primary infection with one of the four DENV serotypes typically confers antibody-mediated lifelong protection against reinfection with the same serotype. Primary DENV infection may protect against, have no effect on, or enhance subsequent infection with a heterotypic serotype [7]. Reinfection with a heterotypic DENV serotype is associated with higher viral load and an elevated risk of dengue hemorrhagic fever (DHF) and dengue shock syndrome (DSS) [8]. Secondary DENV infections in macaques share some similarities with human infections including a trend toward higher peak DENV viral load [9]. A single rhesus macaque was previously reported as developing clinical responses consistent with dengue fever/DSS in response to secondary DENV-2 infection, including leukocytosis, thrombocytopenia, and elevated hematocrit approximately 5 days after viremia was first detected [9]

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