基于水疱性口炎病毒的苏丹病毒疫苗的种属特异性免疫原性和保护效力:猕猴挑战研究。
Species-specific immunogenicity and protective efficacy of a vesicular stomatitis virus-based Sudan virus vaccine: a challenge study in macaques.
机构信息
Laboratory of Virology, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rocky Mountain Laboratories, Hamilton, MT, USA.
Laboratory of Virology, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rocky Mountain Laboratories, Hamilton, MT, USA.
出版信息
Lancet Microbe. 2023 Mar;4(3):e171-e178. doi: 10.1016/S2666-5247(23)00001-0. Epub 2023 Feb 2.
BACKGROUND
The recent Sudan virus (SUDV) outbreak in Uganda highlights the need for rapid response capabilities, including development of vaccines against emerging viruses with high public health impact. We aimed to develop a Sudan virus-specific vaccine suitable for emergency use during outbreaks.
METHODS
We generated and characterised a vesicular stomatitis virus (VSV)-based vaccine, VSV- SUDV, and evaluated the protective efficacy following a single-dose vaccination against lethal SUDV infection in non-human primates (NHPs). We used male and female cynomolgus macaques (n=11) aged 6-11 years and weighing 3·8-9·0 kg. Animals received a 1 mL intramuscular injection for vaccination containing either 1 × 10 plaque forming units (PFU) VSV-SUDV or 1 × 10 PFU of a VSV-based vaccine against Marburg virus (control; five NHPs). NHPs were challenged intramuscularly 28 days after vaccination with 1 × 10 TCID SUDV-Gulu. We assessed anaesthetised NHPs on days 28, 21, 14, and 7 before challenge; days 0, 3, 6, 9, 14, 21, 28, and 35 after challenge; and at euthanasia (day 40 for survivors). As we repurposed NHPs from a successful VSV-Ebola virus (EBOV) vaccine efficacy study, we also investigated VSV-EBOV's cross-protective potential against SUDV challenge.
FINDINGS
Of the six NHPs given VSV-SUDV, none showed any signs of disease in response to the challenge. Four of the five NHPs in the control group developed characteristic clinical signs of Sudan virus diseases. SUDV glycoprotein-specific IgG concentrations peaked 14 days after vaccination (titre of >1:10 000) and reached their highest concentrations at 6 days after challenge (1:25 600-1:102 400). Although the NHPs developed cross-reactive humoral responses to SUDV after VSV-EBOV vaccination and EBOV challenge, there was little cross-protection.
INTERPRETATION
These data emphasise the need for species-specific vaccines for each human-pathogenic Ebolavirus. Furthermore, although previous VSV-EBOV immunity is boosted through VSV-SUDV vaccination, it only has a small effect on the immunogenicity and protective efficacy of VSV-SUDV vaccination against SUDV challenge.
FUNDING
Intramural Research Program, US National Institute of Allergy and Infectious Diseases, National Institutes of Health.
背景
最近在乌干达爆发的苏丹病毒(SUDV)突显了快速应对能力的必要性,包括开发针对具有高公共卫生影响的新兴病毒的疫苗。我们旨在开发一种适用于爆发期间紧急使用的苏丹病毒特异性疫苗。
方法
我们生成并表征了一种基于水疱性口炎病毒(VSV)的疫苗,VSV-SUDV,并在非人类灵长类动物(NHP)中评估了单次接种疫苗对致死性 SUDV 感染的保护效力。我们使用了 6-11 岁、体重 3.8-9.0kg 的雄性和雌性食蟹猴(n=11)。动物接受含 1×10 个噬菌斑形成单位(PFU)VSV-SUDV 或 1×10 个 PFU 针对马尔堡病毒的基于 VSV 的疫苗(对照;5 只 NHP)的 1mL 肌内注射进行疫苗接种。接种后 28 天,NHP 经肌内挑战 1×10 TCID SUDV-Gulu。我们在挑战前的第 28、21、14 和 7 天以及挑战后的第 0、3、6、9、14、21、28 和 35 天以及 40 天(幸存者)对麻醉的 NHP 进行评估。由于我们从成功的 VSV-埃博拉病毒(EBOV)疫苗功效研究中重新利用了 NHP,因此我们还研究了 VSV-EBOV 对 SUDV 挑战的交叉保护潜力。
发现
在接受 VSV-SUDV 治疗的六只 NHP 中,没有一只对挑战表现出任何疾病迹象。对照组中的五只 NHP 中有四只出现了苏丹病毒病的特征性临床症状。SUDV 糖蛋白特异性 IgG 浓度在接种后 14 天达到峰值(>1:10000),并在接种后 6 天达到最高浓度(1:25600-1:102400)。尽管 NHP 在接受 VSV-EBOV 疫苗接种和 EBOV 挑战后产生了针对 SUDV 的交叉反应性体液反应,但交叉保护作用很小。
解释
这些数据强调了针对每种人类致病性埃博拉病毒的种特异性疫苗的必要性。此外,尽管先前的 VSV-EBOV 免疫通过 VSV-SUDV 疫苗接种得到增强,但它对 VSV-SUDV 疫苗接种对 SUDV 挑战的免疫原性和保护效力的影响很小。
资金
美国国立过敏和传染病研究所,美国国立卫生研究院内部研究计划。
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