Abstract

BackgroundLassa hemorrhagic fever (LHF) is a rodent-borne viral disease that can be fatal for human beings. In this study, an attenuated Lassa vaccine candidate, ML29, was tested in SIV-infected rhesus macaques for its ability to elicit immune responses without instigating signs pathognomonic for arenavirus disease. ML29 is a reassortant between Lassa and Mopeia viruses that causes a transient infection in non-human primates and confers sterilizing protection from lethal Lassa viral challenge. However, since the LHF endemic area of West Africa also has high HIV seroprevalence, it is important to determine whether vaccination could be safe in the context of HIV infection.ResultsSIV-infected and uninfected rhesus macaques were vaccinated with the ML29 virus and monitored for specific humoral and cellular immune responses, as well as for classical and non-classical signs of arenavirus disease. Classical disease signs included viremia, rash, respiratory distress, malaise, high liver enzyme levels, and virus invasion of the central nervous system. Non-classical signs, derived from profiling the blood transcriptome of virulent and non-virulent arenavirus infections, included increased expression of interferon-stimulated genes (ISG) and decreased expression of COX2, IL-1β, coagulation intermediates and nuclear receptors needed for stress signaling. All vaccinated monkeys showed ML29-specific antibody responses and ML29-specific cell-mediated immunity.ConclusionSIV-infected and uninfected rhesus macaques responded similarly to ML29 vaccination, and none developed chronic arenavirus infection. Importantly, none of the macaques developed signs, classical or non-classical, of arenavirus disease.

Highlights

  • Lassa hemorrhagic fever (LHF) is a rodent-borne viral disease that can be fatal for human beings

  • 393 days after infection with SIVmac251, eleven rhesus macaques were enrolled in this study

  • Eight macaques were inoculated with an attenuated Lassa virus (LASV) vaccine ML-29, in order to determine whether they could still elicit LASVspecific immune responses without developing signs of arenavirus disease

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Summary

Introduction

Lassa hemorrhagic fever (LHF) is a rodent-borne viral disease that can be fatal for human beings. Since the LHF endemic area of West Africa has high HIV seroprevalence, it is important to determine whether vaccination could be safe in the context of HIV infection. Lassa hemorrhagic fever (LHF) is a rodent-transmitted disease that causes more than 300,000 human cases per year in the West African endemic area. Mortality rates are between 15-20% in hospitalized individuals, and reach 50% in epidemic episodes [1,2]. Those who develop effective antiviral immunity survive, while those with uncontrolled high viral loads succumb [3,4,5]. Due to the undifferentiated symptoms at the onset of LHF, the opportunity to administer ribavirin treatment is often missed; so the best public health option in endemic areas would be vaccination

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