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本文引用的文献

1
Postexposure protection against Marburg haemorrhagic fever with recombinant vesicular stomatitis virus vectors in non-human primates: an efficacy assessment.非人灵长类动物中使用重组水疱性口炎病毒载体进行马尔堡出血热暴露后预防:疗效评估
Lancet. 2006 Apr 29;367(9520):1399-404. doi: 10.1016/S0140-6736(06)68546-2.
2
Renewed promise. Annual AIDS vaccine meeting highlights recent data from clinical trials and lessons on recruitment and retention of volunteers.新的希望。年度艾滋病疫苗会议突出了近期临床试验数据以及志愿者招募和留存方面的经验教训。
IAVI Rep. 2005 Sep-Oct;9(4):18-20.
3
A single-cycle vaccine vector based on vesicular stomatitis virus can induce immune responses comparable to those generated by a replication-competent vector.一种基于水疱性口炎病毒的单周期疫苗载体能够诱导出与具备复制能力的载体所产生的免疫反应相当的免疫反应。
J Virol. 2005 Nov;79(21):13231-8. doi: 10.1128/JVI.79.21.13231-13238.2005.
4
Development of a new vaccine for the prevention of Lassa fever.开发一种预防拉沙热的新型疫苗。
PLoS Med. 2005 Jun;2(6):e183. doi: 10.1371/journal.pmed.0020183. Epub 2005 Jun 28.
5
Live attenuated recombinant vaccine protects nonhuman primates against Ebola and Marburg viruses.减毒活重组疫苗可保护非人灵长类动物免受埃博拉病毒和马尔堡病毒感染。
Nat Med. 2005 Jul;11(7):786-90. doi: 10.1038/nm1258. Epub 2005 Jun 5.
6
Marburg haemorrhagic fever, Angola.安哥拉马尔堡出血热
Wkly Epidemiol Rec. 2005 May 6;80(18):158-9.
7
Properties of replication-competent vesicular stomatitis virus vectors expressing glycoproteins of filoviruses and arenaviruses.表达丝状病毒和沙粒病毒糖蛋白的具有复制能力的水疱性口炎病毒载体的特性
J Virol. 2004 May;78(10):5458-65. doi: 10.1128/jvi.78.10.5458-5465.2004.
8
Organisation of health care during an outbreak of Marburg haemorrhagic fever in the Democratic Republic of Congo, 1999.1999年刚果民主共和国马尔堡出血热疫情期间的医疗保健组织情况
J Infect. 2004 May;48(4):347-53. doi: 10.1016/S0163-4453(03)00122-1.
9
Current Assessment of Yellow Fever and Yellow Fever Vaccine.黄热病及黄热病疫苗的当前评估
Curr Infect Dis Rep. 2004 Apr;6(2):96-104. doi: 10.1007/s11908-996-0005-9.
10
Accelerated vaccination for Ebola virus haemorrhagic fever in non-human primates.非人灵长类动物埃博拉病毒出血热的加速疫苗接种
Nature. 2003 Aug 7;424(6949):681-4. doi: 10.1038/nature01876.

使用减毒活重组疫苗对马尔堡病毒株进行交叉保护。

Cross-protection against Marburg virus strains by using a live, attenuated recombinant vaccine.

作者信息

Daddario-DiCaprio Kathleen M, Geisbert Thomas W, Geisbert Joan B, Ströher Ute, Hensley Lisa E, Grolla Allen, Fritz Elizabeth A, Feldmann Friederike, Feldmann Heinz, Jones Steven M

机构信息

Virology Division, USAMRIID, Fort Detrick, MD 21702-5011, USA.

出版信息

J Virol. 2006 Oct;80(19):9659-66. doi: 10.1128/JVI.00959-06.

DOI:10.1128/JVI.00959-06
PMID:16973570
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1617222/
Abstract

Marburg virus (MARV) has been associated with sporadic episodes of hemorrhagic fever, including a recent highly publicized outbreak in Angola that produced severe disease and significant mortality in infected patients. MARV is also considered to have potential as a biological weapon. Recently, we reported the development of a promising attenuated, replication-competent vaccine against MARV based on recombinant vesicular stomatitis virus (VSV) expressing the glycoprotein of the Musoke strain of MARV (VSVDeltaG/MARVGP-Musoke). We used this vaccine to demonstrate complete protection of cynomolgus monkeys against a homologous MARV challenge. While these results are highly encouraging, an effective vaccine would need to confer protection against all relevant strains of MARV. Here, we evaluated the protective efficacy of the VSVDeltaG/MARVGP-Musoke vaccine against two heterologous MARV strains, the seemingly more pathogenic Angola strain and the more distantly related Ravn strain. In this study, seven cynomolgus monkeys were vaccinated with the VSVDeltaG/MARVGP-Musoke vector. Three of these animals were challenged with the Angola strain, three with the Ravn strain, and a single animal with the Musoke strain of MARV. Two animals served as controls and were each injected with a nonspecific VSV vector; these controls were challenged with the Angola and Ravn strains, respectively. Both controls succumbed to challenge by day 8. However, none of the specifically vaccinated animals showed any evidence of illness either from the vaccination or from the MARV challenges and all of these animals survived. These data suggest that the VSVDeltaG/MARVGP-Musoke vaccine should be sufficient to protect against all known MARV strains.

摘要

马尔堡病毒(MARV)与散发性出血热疫情有关,包括最近在安哥拉爆发的一次备受关注的疫情,该疫情导致感染患者出现严重疾病并造成大量死亡。MARV还被认为具有作为生物武器的潜力。最近,我们报道了一种有前景的基于表达马尔堡病毒穆索凯株糖蛋白的重组水疱性口炎病毒(VSV)的减毒、有复制能力的抗MARV疫苗(VSVDeltaG/MARVGP - 穆索凯)的研发。我们使用这种疫苗证明了食蟹猴能完全抵御同源MARV攻击。虽然这些结果非常令人鼓舞,但一种有效的疫苗需要对所有相关的MARV毒株都提供保护。在此,我们评估了VSVDeltaG/MARVGP - 穆索凯疫苗对两种异源MARV毒株的保护效力,即看似致病性更强的安哥拉毒株和亲缘关系更远的拉夫恩毒株。在本研究中,七只食蟹猴用VSVDeltaG/MARVGP - 穆索凯载体进行了疫苗接种。其中三只动物用安哥拉毒株进行攻击,三只用拉夫恩毒株进行攻击,还有一只用MARV的穆索凯毒株进行攻击。两只动物作为对照,分别注射非特异性VSV载体;这些对照分别用安哥拉毒株和拉夫恩毒株进行攻击。两个对照组在第8天均死于攻击。然而,所有经过特异性疫苗接种的动物无论是接种疫苗还是受到MARV攻击后均未表现出任何患病迹象,并且所有这些动物都存活了下来。这些数据表明,VSVDeltaG/MARVGP - 穆索凯疫苗应该足以抵御所有已知的MARV毒株。