A Recombinant Vesicular Stomatitis Virus Ebola Vaccine

Regules, Jason A.; Beigel, John H.; Paolino, Kristopher; Voell, Jocelyn; Castellano, Amy R.; Hu, Zonghui; Muñoz, P. Rubio; Moon, James E.; Ruck, Richard C.; Bennett, Jason; Twomey, Patrick; Gutiérrez, Ramiro L.; Remich, Shon; Hack, Holly R.; Wisniewski, Meagan L.; Josleyn, Matthew; Kwilas, Steven A.; Deusen, Nicole Van; Mbaya, Olivier Tshiani; Zhou, Yan; Stanley, Daphne A.; Wang, Jing; Smith, Kirsten S.; Shi, M.; Ledgerwood, Julie E.; Graham, Barney S.; Sullivan, Nancy J.; Jagodzinski, Linda L.; Peel, Sheila A.; Alimonti, Judie B.; Hooper, Jay W.; Silvera, Peter; Martin, Brian K.; Monath, Thomas P.; Ramsey, W. Jay; Link, Charles J.; Lane, H. Clifford; Michael, Nelson L.; Davey, Richard T.; Thomas, Stephen J.

doi:10.1056/nejmoa1414216

Cited by 334 publications

(306 citation statements)

References 25 publications

(30 reference statements)

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“…Vaccines that were assessed in phase I and/or II studies during the 2013-2016 EBOV epidemic include rVSV-EBOV [268][269][270][271][272] , Ad5-EBOV [273][274][275] , rVSV-EBOV combined with rAd5-EBOV 276 , ChAd3-EBOV with or without MVA-EBOV [277][278][279][280] , Ad26-EBOV combined with MVA-EBOV 281 , and DNA encoding multiple filovirus GPs 282,283 . These EBOV vaccines generally elicited good immunogenicity against EBOV GP, and no serious adverse events were described.…”

Section: Vaccination Of Humansmentioning

confidence: 99%

Post-exposure treatments for Ebola and Marburg virus infections

Cross

Mire

Feldmann

et al. 2018

Nat Rev Drug Discov

106

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| The filoviruses -Ebola virus and Marburg virus -cause lethal haemorrhagic fever in humans and non-human primates (NHPs). Filoviruses present a global health threat both as naturally acquired diseases and as potential agents of bioterrorism. In the recent 2013-2016 outbreak of Ebola virus, the most promising therapies for post-exposure use with demonstrated efficacy in the gold-standard NHP models of filovirus disease were unable to show statistically significant protection in patients infected with Ebola virus. This Review briefly discusses these failures and what has been learned from these experiences, and summarizes the current status of post-exposure medical countermeasures in development, including antibodies, small interfering RNA and small molecules. We outline how our current knowledge could be applied to the identification of novel interventions and ways to use interventions more effectively. R E V I E W SNATURE REVIEWS | DRUG DISCOVERY VOLUME 17 | JUNE 2018 | 413 © 2 0 1 8 M a c m i l l a n P u b l i s h e r s L i m i t e d , p a r t o f S p r i n g e r N a t u r e . A l l r i g h t s r e s e r v e d . AstheniaMuscular weakness. MyalgiaMuscular pain. ArthralgiaJoint pain. LeukopeniaA condition of having a low number of circulating leukocytes, including neutrophils, eosinophils, basophils, lymphocytes and monocytes. LymphocytopeniaA condition of having a low number of circulating leukocytes, including natural killer cells, T cells and B cells. ThrombocytopeniaA condition of having a low number of circulating thrombocytes, also known as platelets.and Ebolavirus. The Marburgvirus genus contains a single species, Marburg marburgvirus, which contains two members, Marburg virus (MARV) and Ravn virus (RAVV). The Ebolavirus genus consists of five distinct species: Bundibugyo ebolavirus (BDBV), Reston ebolavirus (RESTV), Sudan ebolavirus (SUDV), Tai Forest ebolavirus (TAFV; previously termed 'Côte d'Ivoire ebolavirus' but more commonly known as 'Ivory Coast ebolavirus') and Zaire ebolavirus (EBOV). MARV, RAVV, BDBV, SUDV and EBOV are important human pathogens, with case fatality rates often up to 90% for MARV, RAVV and EBOV, and around 55% for SUDV 8,10 . On the basis of two small outbreaks in 2007 and 2012, BDBV seems to be the least pathogenic, with a case fatality rate of about 40-48% 11,12 . In 1994, TAFV was associated with a number of deaths in chimpanzees and a single symptomatic but non-lethal human infection in the Republic of Côte d'Ivoire 13,14 . RESTV is lethal for macaques but is not thought to cause disease in humans 15 . An outbreak of RESTV was reported in pigs in the Philippines in 2008; however, it remains uncertain whether the disease observed in the pigs was caused by RESTV or other agents reported to have co-infected the animals 16 . Clinical manifestationsClinical and laboratory signs of disease caused by filovirus infection are nonspecific and usually associated with an incubation period of 2-21 days (mean 4-10 days) 8,17 . Illness begins with an abrupt onset of fever, astheni...

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Section: Vaccination Of Humansmentioning

confidence: 99%

Post-exposure treatments for Ebola and Marburg virus infections

Cross

Mire

Feldmann

et al. 2018

Nat Rev Drug Discov

106

View full text Add to dashboard Cite

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“…Early results on humoral and cell-mediated responses of ChAd3-EBOV were promising overall, although somewhat mixed (12,13), and similarly encouraging humoral responses to rVSV-ZEBOV were found at day 28 after vaccination (14). These small studies of both vaccines had not detected any safety issues, but in midDecember 2014, a phase I study under way in Switzerland that used rVSV-ZEBOV was paused to assess episodes of reported arthritis that began during the second week after vaccination.…”

Section: Vaccine Selectionmentioning

confidence: 99%

“…In early January 2015, the study was resumed at a lower dose of vaccine (15). Investigators of other phase I studies in the United States examined their data but did not initially detect similar adverse events (14), although an association was detected later in some other trials also.…”

Section: Vaccine Selectionmentioning

confidence: 99%

Implementing an Ebola Vaccine Study — Sierra Leone

et al. 2016

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“…Currently trial success was exhibited with the VSV-ZEBOV recombinant, live attenuated, replicationcompetent genetically engineered vesicular stomatitis virus vaccine (Regules et al, 2015;Henao-Restrepo et Kashangura 55 al., 2017). The vaccine candidate (rVSV-ZEBOV) is genetically engineered to replace the VSV glycoprotein with the glycoprotein from a Zaire strain of Ebola virus (ZEBOV) (Regules et al, 2015).…”

Section: Potential Development Of Anti-ebov Line 1 (Designed Gp Sequementioning

confidence: 99%

Glance at potential future combating of diseases: Bioengineered antimicrobial organisms

Kashangura¹

2017

Sci. Res. Essays

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The incidence of diseases is on the surge as exemplified by the recent occurrence in West Africa of Ebola Virus (EBOV) and increase of Zika Virus in Brazil. These pathogens have evolved strategies to evade the human immune system and thus continue to be globally important human pathogens. Bioengineering capabilities are on the increase with rapid advances in synthetic biology and allied technologies (nanobiotechnology, nanotechnology, OMICs technologies, and genetic engineering) which bring potential future prospects in combating disease causing agents using the knowledge of pathogenesis of these disease causing agents. This paper specifically takes a forward looking approach in proposing a potential future use of bioengineering technologies to combat disease causing pathogens as exemplified by Human Immunodeficiency Virus (HIV), Ebola Virus (EBOV), and Mycobacterium tuberculosis through the design, building and testing of synthetic bioengineered minimal genomes with pathogen neutralising capabilities and pathogen detection sensitivity similar to whole cell based biosensors.

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A Recombinant Vesicular Stomatitis Virus Ebola Vaccine

Cited by 334 publications

References 25 publications

Post-exposure treatments for Ebola and Marburg virus infections

Post-exposure treatments for Ebola and Marburg virus infections

Implementing an Ebola Vaccine Study — Sierra Leone

Glance at potential future combating of diseases: Bioengineered antimicrobial organisms

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