2016
DOI: 10.1080/14760584.2016.1187566
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Ebola virus disease candidate vaccines under evaluation in clinical trials

Abstract: Summary Filoviruses are the etiological agents of two human illnesses: Ebola virus disease and Marburg virus disease. Until 2013, medical countermeasure development against these afflictions was limited to only a few research institutes worldwide as both infections were considered exotic due to very low case numbers. Together with the high case-fatality rate of both diseases, evaluation of any candidate countermeasure in properly controlled clinical trials seemed impossible. However, in 2013, Ebola virus was i… Show more

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Cited by 51 publications
(42 citation statements)
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References 106 publications
(98 reference statements)
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“…Both MARV and EBOV have caused numerous outbreaks throughout Africa, and EBOV is responsible for the 2013–2015 West African epidemic that infected over 28,000 people and left over 11,000 dead (World Health Organization, 2016). No vaccine is currently approved to prevent filovirus disease, although many candidates have shown efficacy in non-human primates as well as in human trials conducted during the West African Ebola epidemic (Feldmann et al, 2013; Martins et al, 2016). Likewise, no drug candidate has been approved for use, but several candidates have been developed, including siRNAs, monoclonal antibodies, interferon, and estrogen receptor modulators (Johansen et al, 2013; Bixler et al, 2017; Connor et al, 2017; Olinger Jr et al, 2012; Qiu et al, 2012).…”
Section: Introductionmentioning
confidence: 99%
“…Both MARV and EBOV have caused numerous outbreaks throughout Africa, and EBOV is responsible for the 2013–2015 West African epidemic that infected over 28,000 people and left over 11,000 dead (World Health Organization, 2016). No vaccine is currently approved to prevent filovirus disease, although many candidates have shown efficacy in non-human primates as well as in human trials conducted during the West African Ebola epidemic (Feldmann et al, 2013; Martins et al, 2016). Likewise, no drug candidate has been approved for use, but several candidates have been developed, including siRNAs, monoclonal antibodies, interferon, and estrogen receptor modulators (Johansen et al, 2013; Bixler et al, 2017; Connor et al, 2017; Olinger Jr et al, 2012; Qiu et al, 2012).…”
Section: Introductionmentioning
confidence: 99%
“…The success of the VSV vectored Ebola Zaire vaccine in human trials implies that vaccines can be made against the other related filoviruses, and there is general agreement that protection should be ensured against at least Ebola Sudan, Bundibugyo, and Marburg viruses. [17][18][19] However, unless fortuitous outbreaks occur we will be unable to demonstrate the efficacy of those other filovirus vaccines except by determination of correlates of protection in 2 relevant animal models or by analogy to human responses to Ebola Zaire vaccine. It is not yet clear how CEPI will choose among the many filovirus candidate vaccines.…”
Section: The Short Term: Filoviruses and Chikungunyamentioning
confidence: 99%
“…A number of candidate vaccines for EBOV have demonstrated protection against lethal EBOV challenge in animal models and progressed to clinical trials, and most of these vaccines, including DNA vaccines [11], vaccines based on viral vectors, such as recombinant adenovirus [12] and vesicular stomatitis virus (VSV) [13], and protein-based vaccines, such as virus-like particles (VLPs) [14], have been based on GP. Most notably, a number of the candidate vaccines currently under clinical phase evaluation are viral vector-based vaccines [15,16]. While recombinant vesicular stomatitis virus (rVSV)-based and recombinant adenovirus type-5 vector (rAd5)-based EBOV candidate vaccines have been shown to be highly efficacious against EBOV infection and transmission, numerous side effects, such as fever, acute arthritis, and skin lesions, have been reported [15,17,18].…”
mentioning
confidence: 99%
“…Most notably, a number of the candidate vaccines currently under clinical phase evaluation are viral vector-based vaccines [15,16]. While recombinant vesicular stomatitis virus (rVSV)-based and recombinant adenovirus type-5 vector (rAd5)-based EBOV candidate vaccines have been shown to be highly efficacious against EBOV infection and transmission, numerous side effects, such as fever, acute arthritis, and skin lesions, have been reported [15,17,18]. In addition, preexisting antibodies, costs, and side effects should also be considered.…”
mentioning
confidence: 99%