Polio endgame risks and the possibility of restarting the use of oral poliovirus vaccine

Tebbens, Radboud J. Duintjer; Thompson, Kimberly M.

doi:10.1080/14760584.2018.1506333

Cited by 41 publications

(53 citation statements)

References 54 publications

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“…Subsequent modelling studies indicated that polio eradication, as compared with control, would be more cost-effective and ultimately incur substantial net benefits 8 9. These studies were, however, criticised as depending on untenable or at least highly optimistic assumptions 10–12…”

Section: Early But Truncated Successmentioning

confidence: 99%

“…The current DRC epidemic has emerged in different provinces as independent cVDPV type 2 outbreaks, which now threatens to spread to other neighbouring countries and may endanger the whole of sub-Saharan Africa (SSA) 3 5. By 2016, 155 countries had already replaced trivalent OPV with a bivalent (types 1 and 3) vaccine; the DRC outbreak thus demonstrates the weaknesses in polio surveillance systems and—if not contained—may cause a general move back to the trivalent OPV 3 4 10 24…”

Section: Challenging Epidemiolgical Developmentsmentioning

confidence: 99%

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Polio: from eradication to systematic, sustained control

et al. 2019

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Section: Early But Truncated Successmentioning

confidence: 99%

Section: Challenging Epidemiolgical Developmentsmentioning

confidence: 99%

Polio: from eradication to systematic, sustained control

et al. 2019

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“…cVDPVs have been designated a Public Health Emergency of International Concern, for which the only effective control is use of stockpiled monovalent OPV2. Use of this vaccine carries the inherent risk of seeding new cVDPVs, particularly with waning mucosal immunity of the population following OPV2 cessation 8, 9. IPV use cannot generate cVDPVs but these vaccines do not induce primary intestinal mucosal immunity, so IPV use is ineffective in interrupting transmission in settings where transmission is predominantly via the faecal–oral route 10, 11.…”

Section: Introductionmentioning

confidence: 99%

The safety and immunogenicity of two novel live attenuated monovalent (serotype 2) oral poliovirus vaccines in healthy adults: a double-blind, single-centre phase 1 study

et al. 2019

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Summary Background Use of oral live-attenuated polio vaccines (OPV), and injected inactivated polio vaccines (IPV) has almost achieved global eradication of wild polio viruses. To address the goals of achieving and maintaining global eradication and minimising the risk of outbreaks of vaccine-derived polioviruses, we tested novel monovalent oral type-2 poliovirus (OPV2) vaccine candidates that are genetically more stable than existing OPVs, with a lower risk of reversion to neurovirulence. Our study represents the first in-human testing of these two novel OPV2 candidates. We aimed to evaluate the safety and immunogenicity of these vaccines, the presence and extent of faecal shedding, and the neurovirulence of shed virus. Methods In this double-blind, single-centre phase 1 trial, we isolated participants in a purpose-built containment facility at the University of Antwerp Hospital (Antwerp, Belgium), to minimise the risk of environmental release of the novel OPV2 candidates. Participants, who were recruited by local advertising, were adults (aged 18–50 years) in good health who had previously been vaccinated with IPV, and who would not have any contact with immunosuppressed or unvaccinated people for the duration of faecal shedding at the end of the study. The first participant randomly chose an envelope containing the name of a vaccine candidate, and this determined their allocation; the next 14 participants to be enrolled in the study were sequentially allocated to this group and received the same vaccine. The subsequent 15 participants enrolled after this group were allocated to receive the other vaccine. Participants and the study staff were masked to vaccine groups until the end of the study period. Participants each received a single dose of one vaccine candidate (candidate 1, S2/cre5/S15domV/rec1/hifi3; or candidate 2, S2/S15domV/CpG40), and they were monitored for adverse events, immune responses, and faecal shedding of the vaccine virus for 28 days. Shed virus isolates were tested for the genetic stability of attenuation. The primary outcomes were the incidence and type of serious and severe adverse events, the proportion of participants showing viral shedding in their stools, the time to cessation of viral shedding, the cell culture infective dose of shed virus in virus-positive stools, and a combined index of the prevalence, duration, and quantity of viral shedding in all participants. This study is registered with EudraCT, number 2017-000908-21 and ClinicalTrials.gov , number NCT03430349 . Findings Between May 22 and Aug 22, 2017, 48 volunteers were screened, of whom 15 (31%) volunteers were excluded for reasons relating to the inclusion or exclusion criteria, three (6%) volunteers were not treated because of restrictions to the number of participants in each group, and 30 (63%) volunteers were sequentially allocated to groups (15 participants per group). Both no...

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“…In our model, the total (‘all serotypes’) would continue to increase until the last OPV cessation. In addition to these possibilities, OPV2 cessation did not go as smoothly as hoped, and the use of monovalent OPV2 continues to date (as of August 2019) in response to cVDPV2 outbreaks[54]. This means that the model should include the possibility of creating some new iVDPV2 excreters in the areas of serotype 2 outbreaks.…”

Section: Discussionmentioning

confidence: 99%

Updated modelling of the prevalence of immunodeficiency-associated long-term vaccine-derived poliovirus (iVDPV) excreters

Kalkowska¹,

Pallansch

Thompson³

2019

Epidemiol. Infect.

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Conditions and evidence continue to evolve related to the prediction of the prevalence of immunodeficiency-associated long-term vaccine-derived poliovirus (iVDPV) excreters, which affect assumptions related to forecasting risks and evaluating potential risk management options. Multiple recent reviews provided information about individual iVDPV excreters, but inconsistencies among the reviews raise some challenges. This analysis revisits the available evidence related to iVDPV excreters and provides updated model estimates that can support future risk management decisions. The results suggest that the prevalence of iVDPV excreters remains highly uncertain and variable, but generally confirms the importance of managing the risks associated with iVDPV excreters throughout the polio endgame in the context of successful cessation of all oral poliovirus vaccine use.

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Polio endgame risks and the possibility of restarting the use of oral poliovirus vaccine

Cited by 41 publications

References 54 publications

Polio: from eradication to systematic, sustained control

Polio: from eradication to systematic, sustained control

The safety and immunogenicity of two novel live attenuated monovalent (serotype 2) oral poliovirus vaccines in healthy adults: a double-blind, single-centre phase 1 study

Updated modelling of the prevalence of immunodeficiency-associated long-term vaccine-derived poliovirus (iVDPV) excreters

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