mRNA 疫苗对具有大流行潜力的 H10N8 和 H7N9 流感病毒具有免疫原性,在 1 期随机临床试验中,健康成年人中具有良好的耐受性。
mRNA vaccines against H10N8 and H7N9 influenza viruses of pandemic potential are immunogenic and well tolerated in healthy adults in phase 1 randomized clinical trials.
机构信息
Miami Research Associates, 6280 Sunset Drive, Suite 600, So. Miami, FL 33143, USA.
PAREXEL International GmbH Klinikum Westend, House 18, Spandauer Damm 130, 14050 Berlin, Germany.
出版信息
Vaccine. 2019 May 31;37(25):3326-3334. doi: 10.1016/j.vaccine.2019.04.074. Epub 2019 May 10.
BACKGROUND
We evaluated safety and immunogenicity of the first mRNA vaccines against potentially pandemic avian H10N8 and H7N9 influenza viruses.
METHODS
Two randomized, placebo-controlled, double-blind, phase 1 clinical trials enrolled participants between December 2015 and August 2017 at single centers in Germany (H10N8) and USA (H7N9). Healthy adults (ages 18-64 years for H10N8 study; 18-49 years for H7N9 study) participated. Participants received vaccine or placebo in a 2-dose vaccination series 3 weeks apart. H10N8 intramuscular (IM) dose levels of 25, 50, 75, 100, and 400 µg and intradermal dose levels of 25 and 50 µg were evaluated. H7N9 IM 10-, 25-, and 50-µg dose levels were evaluated; 2-dose series 6 months apart was also evaluated. Primary endpoints were safety (adverse events) and tolerability. Secondary immunogenicity outcomes included humoral (hemagglutination inhibition [HAI], microneutralization [MN] assays) and cell-mediated responses (ELISPOT assay).
RESULTS
H10N8 and H7N9 mRNA IM vaccines demonstrated favorable safety and reactogenicity profiles. No vaccine-related serious adverse event was reported. For H10N8 (N = 201), 100-µg IM dose induced HAI titers ≥ 1:40 in 100% and MN titers ≥ 1:20 in 87.0% of participants. The 25-µg intradermal dose induced HAI titers > 1:40 in 64.7% of participants compared to 34.5% of participants receiving the IM dose. For H7N9 (N = 156), IM doses of 10, 25, and 50 µg achieved HAI titers ≥ 1:40 in 36.0%, 96.3%, and 89.7% of participants, respectively. MN titers ≥ 1:20 were achieved by 100% in the 10- and 25-µg groups and 96.6% in the 50-µg group. Seroconversion rates were 78.3% (HAI) and 87.0% (MN) for H10N8 (100 µg IM) and 96.3% (HAI) and 100% (MN) in H7N9 (50 µg). Significant cell-mediated responses were not detected in either study.
CONCLUSIONS
The first mRNA vaccines against H10N8 and H7N9 influenza viruses were well tolerated and elicited robust humoral immune responses. ClinicalTrials.gov NCT03076385 and NCT03345043.
背景
我们评估了针对潜在大流行的禽源 H10N8 和 H7N9 流感病毒的首个人mRNA 疫苗的安全性和免疫原性。
方法
2015 年 12 月至 2017 年 8 月,在德国(H10N8 研究)和美国(H7N9 研究)的单个中心进行了两项随机、安慰剂对照、双盲、1 期临床试验。纳入年龄在 18-64 岁(H10N8 研究)和 18-49 岁(H7N9 研究)的健康成年人。参与者接受 3 周间隔的 2 剂疫苗接种系列。评估了 H10N8 肌内(IM)剂量 25、50、75、100 和 400µg 和皮内剂量 25 和 50µg。评估了 H7N9 IM 10、25 和 50µg 剂量水平;还评估了相隔 6 个月的 2 剂系列。主要终点是安全性(不良事件)和耐受性。次要免疫原性结局包括体液(血凝抑制[HAI]、微量中和[MN]测定)和细胞介导的反应(ELISPOT 测定)。
结果
H10N8 和 H7N9 mRNA IM 疫苗表现出良好的安全性和反应原性特征。没有报告与疫苗相关的严重不良事件。对于 H10N8(N=201),100µg IM 剂量诱导的 HAI 滴度≥1:40 在 100%的参与者中和 MN 滴度≥1:20 在 87.0%的参与者中。25µg 皮内剂量在 64.7%的参与者中诱导的 HAI 滴度>1:40,而在接受 IM 剂量的参与者中为 34.5%。对于 H7N9(N=156),10、25 和 50µg 的 IM 剂量分别在 36.0%、96.3%和 89.7%的参与者中达到 HAI 滴度≥1:40。10-和 25-µg 组的 MN 滴度均达到 1:20,而 50-µg 组达到 96.6%。H10N8(100µg IM)的血清转化率为 78.3%(HAI)和 87.0%(MN),H7N9(50µg)为 96.3%(HAI)和 100%(MN)。在两项研究中均未检测到显著的细胞介导反应。
结论
针对 H10N8 和 H7N9 流感病毒的首个人 mRNA 疫苗具有良好的耐受性,并引起了强烈的体液免疫反应。临床试验.gov NCT03076385 和 NCT03345043。
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