Bioprotection Systems, NewLink Genetics, Ames, IA, USA; Devens, MA, USA.
Bioprotection Systems, NewLink Genetics, Ames, IA, USA; Devens, MA, USA.
Lancet Infect Dis. 2017 Aug;17(8):854-866. doi: 10.1016/S1473-3099(17)30313-4. Epub 2017 Jun 9.
The 2014 Zaire Ebola virus outbreak highlighted the need for a safe, effective vaccine with a rapid onset of protection. We report the safety and immunogenicity of the recombinant vesicular stomatitis virus-Zaire Ebola virus envelope glycoprotein vaccine (rVSV∆G-ZEBOV-GP) across a 6 log dose range in two sequential cohorts.
In this phase 1b double-blind, placebo-controlled, dose-response study we enrolled and randomly assigned healthy adults (aged 18-61 years) at eight study sites in the USA to receive a single injection of vaccine or placebo, administered by intramuscular injection. In cohort 1, participants were assigned to receive 3 × 10, 3 × 10, 3 × 10, or 3 × 10 PFU doses of rVSV∆G-ZEBOV-GP or placebo. In cohort 2, participants were assigned to receive 3 × 10, 9 × 10, 2 × 10, or 1 × 10 PFU doses of rVSV∆G-ZEBOV-GP or placebo. Participants were centrally allocated by the study statistician to vaccine groups or placebo through computer-generated randomisation lists. The primary safety outcome was incidence of adverse events within 14 days in the modified intention-to-treat population (all randomly assigned participants who received vaccine or placebo), and the primary outcome for immunogenicity was IgG ELISA antibody titres at day 28 in the per-protocol population. Surveillance was enhanced for arthritis and dermatitis through to day 56. This study is registered with ClinicalTrials.gov, number NCT02314923.
Between Dec 26, 2014, and June 8, 2015, 513 participants were enrolled and randomly assigned; one was not immunised because of unsuccessful phlebotomy. In cohort 1, 256 participants received vaccine (3 × 10 [n=64], 3 × 10 [n=64], 3 × 10 [n=64], or 3 × 10 PFU [n=64]) and 74 received placebo. In cohort 2, 162 participants received vaccine (3 × 10 [n=20], 9 × 10 [n=47], 2 × 10 [n=47], or 1 × 10 PFU [n=48]) and 20 received placebo. Most adverse events occurred in the first day after vaccination, and were mild to moderate in intensity, of a short duration, and more frequent at high vaccine doses (9 × 10 PFU and greater). At the 2 × 10 PFU dose (used in phase 3 trials), the most common local adverse events versus placebo within the first 14 days were arm pain (57·4% [27 of 47] vs 7·4% [seven of 94]) and local tenderness (59·6% [28 of 47] vs 8·5% [eight of 94]). The most common systemic adverse events at the 2 × 10 PFU dose versus placebo, occurring in the first 14 days, were headache (46·8% [22 of 47] vs 27·7% [26 of 94]), fatigue (38·3% [18 of 47] vs 19·1% [18 of 94]), myalgia (34·0% [16 of 47] vs 10·6% [10 of 94]), subjective fever (29·8% [14 of 47] vs 2·1% [two of 94]), shivering or chills (27·7% [13 of 47] vs 7·4% [seven of 94]), sweats (23·4% [11 of 47] vs 3·2% [three of 94]), joint aches and pain (19·1% [nine of 47] vs 7·4% [seven of 94]), objective fever (14·9% [seven of 47] vs 1·1% [one of 94]), and joint tenderness or swelling (14·9% [seven of 47] vs 2·1% [two of 94]). Self-limited, post-vaccination arthritis occurred in 4·5% (19 of 418) of vaccinees (median onset 12·0 days [IQR 10-14]; median duration 8·0 days [6-15]) versus 3·2% (three of 94) of controls (median onset 15·0 days [6-20]; median duration 47·0 days [37-339]), with no apparent dose relationship. Post-vaccination dermatitis occurred in 5·7% (24 of 418) of vaccinees (median onset 9·0 days [IQR 2-12]; median duration 7·0 days [4-9]) versus 3·2% (three of 94) of controls (median onset 5·0 days [3-53]; median duration 33·0 days [5-370]). A low-level, transient, dose-dependent viraemia occurred in concert with early reactogenicity. Antibody responses were observed in most participants by day 14. IgG and neutralising antibody titres were dose-related (p=0·0003 for IgG ELISA and p<0·0001 for the 60% plaque-reduction neutralisation test [PRNT60] by linear trend). On day 28 at the 2 × 10 PFU dose, the geometric mean IgG ELISA endpoint titre was 1624 (95% CI 1146-2302) and seroconversion was 95·7% (95% CI 85·5-98·8); the geometric mean neutralising antibody titre by PRNT60 was 250 (176-355) and seroconversion was 95·7% (85·5-98·8). These robust immunological responses were sustained for 1 year.
rVSV∆G-ZEBOV-GP was well tolerated and stimulated a rapid onset of binding and neutralising antibodies, which were maintained through to day 360. The immunogenicity results support selection of the 2 × 10 PFU dose.
Biomedical Advanced Research and Development Authority, US Department of Health and Human Services.
2014 年扎伊尔埃博拉病毒疫情凸显了需要一种安全、有效且能快速产生保护作用的疫苗。我们报告了重组水疱性口炎病毒-扎伊尔埃博拉病毒包膜糖蛋白疫苗(rVSV∆G-ZEBOV-GP)在两个连续队列中进行的 6 对数剂量范围内的安全性和免疫原性。
在这项 1b 期双盲、安慰剂对照、剂量反应研究中,我们在 8 个美国研究地点招募并随机分配了健康成年人(18-61 岁),接受单次肌内注射疫苗或安慰剂。在队列 1 中,参与者被分配接受 3×10、3×10、3×10 或 3×10 PFU 的 rVSV∆G-ZEBOV-GP 或安慰剂。在队列 2 中,参与者被分配接受 3×10、9×10、2×10 或 1×10 PFU 的 rVSV∆G-ZEBOV-GP 或安慰剂。通过计算机生成的随机分配列表,研究统计学家将参与者中央分配到疫苗组或安慰剂组。主要安全性结局是改良意向治疗人群(所有接受疫苗或安慰剂的随机分配参与者)在 14 天内不良事件的发生率,主要免疫原性结局是在方案人群中第 28 天的 IgG ELISA 抗体滴度。通过加强关节炎和皮疹的监测,直至第 56 天。这项研究在 ClinicalTrials.gov 注册,编号为 NCT02314923。
2014 年 12 月 26 日至 2015 年 6 月 8 日,共纳入 513 名参与者并进行了随机分组;1 人因采血不成功而未免疫。在队列 1 中,256 名参与者接受了疫苗(3×10[64 名]、3×10[64 名]、3×10[64 名]或 3×10 PFU[64 名]),74 名接受了安慰剂。在队列 2 中,162 名参与者接受了疫苗(3×10[20 名]、9×10[47 名]、2×10[47 名]或 1×10 PFU[48 名]),20 名接受了安慰剂。大多数不良事件发生在接种后的第一天,程度为轻至中度,持续时间短,且在高疫苗剂量(9×10 PFU 及以上)时更为常见。在 2×10 PFU 剂量(用于 3 期试验)时,接种后 14 天内,安慰剂组中最常见的局部不良事件是手臂疼痛(47 名中的 57.4%[27 名] vs 94 名中的 7.4%[7 名])和局部压痛(47 名中的 59.6%[28 名] vs 94 名中的 8.5%[8 名])。在 2×10 PFU 剂量下,接种后 14 天内安慰剂组中最常见的全身不良事件是头痛(47 名中的 46.8%[22 名] vs 94 名中的 27.7%[26 名])、疲劳(38.3%[18 名] vs 94 名中的 19.1%[18 名])、肌痛(34.0%[16 名] vs 94 名中的 10.6%[10 名])、主观发热(29.8%[14 名] vs 94 名中的 2.1%[2 名])、寒战或发冷(27.7%[13 名] vs 94 名中的 7.4%[7 名])、出汗(23.4%[11 名] vs 94 名中的 3.2%[3 名])、关节疼痛和疼痛(19.1%[9 名] vs 94 名中的 7.4%[7 名])、客观发热(14.9%[7 名] vs 94 名中的 1.1%[1 名])和关节压痛或肿胀(14.9%[7 名] vs 94 名中的 2.1%[2 名])。接种后关节炎发生在 4.5%(418 名中的 19 名)的疫苗接种者中(中位发病时间 12.0 天[IQR 10-14];中位持续时间 8.0 天[6-15]),而对照组中为 3.2%(94 名中的 3 名)(中位发病时间 15.0 天[6-20];中位持续时间 47.0 天[37-339]),与剂量无关。接种后皮疹发生在 5.7%(418 名中的 24 名)的疫苗接种者中(中位发病时间 9.0 天[IQR 2-12];中位持续时间 7.0 天[4-9]),而对照组中为 3.2%(94 名中的 3 名)(中位发病时间 5.0 天[3-53];中位持续时间 33.0 天[5-370])。在早期反应性的伴随下,出现了低水平、短暂、剂量依赖性的病毒血症。大多数参与者在第 14 天观察到抗体反应。IgG 和中和抗体滴度与剂量相关(IgG ELISA 的 p=0.0003,60%蚀斑减少中和试验[PRNT60]的 p<0.0001 呈线性趋势)。在 2×10 PFU 剂量的第 28 天,几何平均 IgG ELISA 终点滴度为 1624(95%CI 1146-2302),血清转化率为 95.7%(95%CI 85.5-98.8);中和抗体滴度的几何平均 PRNT60 为 250(176-355),血清转化率为 95.7%(85.5-98.8)。这些强大的免疫反应持续了 1 年。
rVSV∆G-ZEBOV-GP 耐受性良好,能迅速产生结合抗体和中和抗体,在第 360 天仍保持稳定。免疫原性结果支持选择 2×10 PFU 剂量。
生物医学高级研究与发展局,美国卫生与公众服务部。
