Pitisuttithum Punnee, Boonnak Kobporn, Chamnanchanunt Supat, Puthavathana Pilaipan, Luvira Viravarn, Lerdsamran Hatairat, Kaewkungwal Jaranit, Lawpoolsri Saranath, Thanachartwet Vipa, Silachamroon Udomsak, Masamae Wanibtisam, Schuetz Alexandra, Wirachwong Ponthip, Thirapakpoomanunt Sit, Rudenko Larisa, Sparrow Erin, Friede Martin, Kieny Marie-Paule
Vaccine Trial Centre, Mahidol University, Bangkok, Thailand.
Vaccine Trial Centre, Mahidol University, Bangkok, Thailand.
Lancet Infect Dis. 2017 Aug;17(8):833-842. doi: 10.1016/S1473-3099(17)30240-2. Epub 2017 May 19.
The emergence of highly pathogenic avian influenza H5N1 viruses has raised concerns about their pandemic potential. Vaccination is the most effective way of preventing influenza. In this study, we investigated the safety and immunogenicity of an avian H5N2 live attenuated influenza vaccine (LAIV H5N2) in healthy Thai adults and its priming immune responses with an H5N1 inactivated vaccine boost.
This study was done at the Vaccine Trial Centre at Mahidol University, Bangkok, Thailand and was divided into two parts. Part 1 consisted of a randomised, double-blind, placebo-controlled trial done over 18 months. We randomly assigned (2:1) healthy Thai adults aged 18-49 years with a computer generated randomisation sequence (blocks of six) to receive either two intranasal doses (0·25 mL per nostril) of LAIV H5N2 (101 participants) or placebo (51 participants) 21 days apart. For part 2, an open-label trial was done in which previously vaccinated participants (40 from LAIV H5N2 group and 20 placebo) were given one intramuscular dose (0·5 mL) of H5N1 booster vaccine. Participants, investigators, and site-study workers were blinded from randomisation. Immune responses after subsequent immunisation were evaluated using haemagglutination-inhibition and microneutralisation assays and circulating follicular T-helper cells and plasmablast cells were measured in serum and whole blood. The trials are registered with ClinicalTrials.gov, numbers NCT01841918 and NCT02229357.
Between Feb 4, 2013, and Feb 28, 2013, 256 individuals were screened, of whom 152 participants were enrolled in part 1 of this study. LAIV H5N2 vaccine was well tolerated. Viral shedding was detected in only six (6%) of 101 participants in the vaccine group 1 day after the first vaccination and in and two (2%) of 98 participants in the group after the second vaccination. There was no serious adverse event in both groups. 51 (50%) of 101 participants in the vaccine group and 28 (55%) of 51 in the placebo group reported at least one adverse event. 80 (84%) of 95 events in the vaccine group and 32 (78%) of 43 events in the placebo groups were reportedly suspected adverse events, probably related to the vaccine; however, most were mild in nature. After two doses of vaccine, 13 (13%) of 100 participants in the vaccine group had an increase in haemagglutination-inhibition titre of more than four-fold and four (4%) of 100 vaccinees developed a rise in neutralisng antibody titre of more than four-fold. 1 year later, after a booster with an inactivated H5N1 vaccine (part 2), 39 (98%) of 40 participants who had previously been vaccinated with LAIV H5N2 had an increase in haemagglutination-inhibition titre of greater than four-fold as early as day 7 compared with three (15%) of 20 participants in the placebo group. Peak geometric mean titre (GMT) for haemagglutination-inhibition antibodies in the previously LAIV H5N2 vaccinated group (566·89 [95% CI 436·97-735·44]) were significantly higher than among those who previously received placebo (25·49 [11·82-54·96]; p<0·0001). The peak GMT by neutralising antibody assay in the H5N2 vaccinated group (1395·85 [1040·79-1872·03]) was also significantly higher than that observed in the placebo group (17·41 [9·05-33·48]; p<0·0001). Importantly, higher cross-reactive haemagglutination-inhibition antibody titres against H5N1 (clades 1, 2.1.3.2, and 2.3.4) were detected in the LAIV H5N2 experienced group than the naive group (p<0·0001).
Our data suggest that LAIV vaccination induces long-lasting memory immune responses. The limitation of this study was that part 2 was designed as a proof-of-concept study by contrast with part 1.
WHO.
高致病性H5N1禽流感病毒的出现引发了人们对其大流行潜力的担忧。接种疫苗是预防流感最有效的方法。在本研究中,我们调查了一种禽H5N2减毒活流感疫苗(LAIV H5N2)在健康泰国成年人中的安全性和免疫原性,以及其与H5N1灭活疫苗加强免疫后的初始免疫反应。
本研究在泰国曼谷玛希隆大学疫苗试验中心进行,分为两个部分。第1部分为一项为期18个月的随机、双盲、安慰剂对照试验。我们使用计算机生成的随机序列(每组6个)将18 - 49岁的健康泰国成年人以2:1的比例随机分配,分别接受两剂鼻内注射(每侧鼻孔0.25 mL)的LAIV H5N2(101名参与者)或安慰剂(51名参与者),间隔21天。对于第2部分,进行了一项开放标签试验,其中先前接种过疫苗的参与者(LAIV H5N2组40名,安慰剂组20名)接受一剂肌肉注射(0.5 mL)的H5N1加强疫苗。参与者、研究者和现场研究人员均对随机分组情况不知情。使用血凝抑制试验和微量中和试验评估后续免疫后的免疫反应,并在血清和全血中测量循环滤泡辅助性T细胞和浆母细胞。这些试验已在ClinicalTrials.gov注册,注册号为NCT01841918和NCT02229357。
在2013年2月4日至2013年2月28日期间,共筛选了256人,其中152名参与者纳入了本研究的第1部分。LAIV H5N2疫苗耐受性良好。在疫苗组的101名参与者中,仅6名(6%)在首次接种疫苗后1天检测到病毒脱落;在第二次接种疫苗后的98名参与者中,有2名(2%)检测到病毒脱落。两组均未出现严重不良事件。疫苗组的101名参与者中有51名(50%)报告至少出现一次不良事件;安慰剂组的51名参与者中有28名(55%)报告至少出现一次不良事件。疫苗组95例不良事件中的80例(84%)和安慰剂组43例不良事件中的32例(78%)据报告为疑似不良事件,可能与疫苗有关;然而,大多数性质轻微。两剂疫苗接种后,疫苗组100名参与者中有13名(13%)的血凝抑制效价升高超过四倍,100名接种者中有4名(4%)产生的中和抗体效价升高超过四倍。1年后,在接受灭活H5N1疫苗加强免疫(第2部分)后,先前接种过LAIV H5N2的40名参与者中有39名(98%)在第7天血凝抑制效价升高超过四倍,而安慰剂组20名参与者中有3名(15%)出现这种情况。先前接种LAIV H5N2的组中血凝抑制抗体的几何平均滴度峰值(GMT)(566.89 [95% CI 436.97 - 735.44])显著高于先前接受安慰剂的组(25.49 [11.82 - 54.96];p<0.0001)。通过中和抗体试验,H5N2疫苗接种组的峰值GMT(1395.85 [1040.79 - 1872.03])也显著高于安慰剂组(17.41 [9.05 - 33.48];p<0.0001)。重要的是,与未接种过疫苗的组相比,LAIV H5N2接种组中检测到针对H5N1(1、2.1.3.2和2.3.4分支)的更高交叉反应血凝抑制抗体效价(p<0.0001)。
我们的数据表明,LAIV疫苗接种可诱导持久的记忆免疫反应。本研究的局限性在于,与第1部分相比,第2部分被设计为一项概念验证研究。
世界卫生组织。
