Live attenuated recombinant vaccine protects nonhuman primates against Ebola and Marburg viruses

被引:0
|
作者
Steven M Jones
Heinz Feldmann
Ute Ströher
Joan B Geisbert
Lisa Fernando
Allen Grolla
Hans-Dieter Klenk
Nancy J Sullivan
Viktor E Volchkov
Elizabeth A Fritz
Kathleen M Daddario
Lisa E Hensley
Peter B Jahrling
Thomas W Geisbert
机构
[1] Special Pathogens Program,Department of Immunology
[2] National Microbiology Laboratory,Department of Medical Microbiology
[3] Public Health Agency of Canada,undefined
[4] University of Manitoba,undefined
[5] University of Manitoba,undefined
[6] United States Army Medical Research Institute of Infectious Diseases,undefined
[7] Institute of Virology,undefined
[8] Philipps-University,undefined
[9] Vaccine Research Center,undefined
[10] National Institute of Allergy and Infectious Diseases,undefined
[11] National Institutes of Health,undefined
[12] Filovirus Laboratory,undefined
[13] University Claude Bernard Lyon-1,undefined
[14] INSERM U412,undefined
[15] Uniformed Services University of the Health Sciences,undefined
来源
Nature Medicine | 2005年 / 11卷
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摘要
Vaccines and therapies are urgently needed to address public health needs stemming from emerging pathogens and biological threat agents such as the filoviruses Ebola virus (EBOV) and Marburg virus (MARV). Here, we developed replication-competent vaccines against EBOV and MARV based on attenuated recombinant vesicular stomatitis virus vectors expressing either the EBOV glycoprotein or MARV glycoprotein. A single intramuscular injection of the EBOV or MARV vaccine elicited completely protective immune responses in nonhuman primates against lethal EBOV or MARV challenges. Notably, vaccine vector shedding was not detectable in the monkeys and none of the animals developed fever or other symptoms of illness associated with vaccination. The EBOV vaccine induced humoral and apparent cellular immune responses in all vaccinated monkeys, whereas the MARV vaccine induced a stronger humoral than cellular immune response. No evidence of EBOV or MARV replication was detected in any of the protected animals after challenge. Our data suggest that these vaccine candidates are safe and highly efficacious in a relevant animal model.
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页码:786 / 790
页数:4
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