Bézay Nicole, Ayad Andrea, Dubischar Katrin, Firbas Christa, Hochreiter Romana, Kiermayr Sigrid, Kiss István, Pinl Fritz, Jilma Bernd, Westritschnig Kerstin
Valneva Austria GmbH, Campus Vienna Biocenter 3, 1030 Vienna, Austria.
Department of Clinical Pharmacology, Medical University of Vienna, Waehringer Guertel 18-20, 1090 Vienna, Austria.
Vaccine. 2016 May 17;34(23):2585-92. doi: 10.1016/j.vaccine.2016.03.098. Epub 2016 Apr 11.
Clostridium difficile infection (CDI) is the leading cause of antibiotic-associated diarrhoea and colitis and the most common pathogen of health care-associated infections. In the US, CDI causes approximately half a million infections and close to 30,000 deaths. Despite antibiotic treatment of C. difficile associated diarrhoea, the disease is complicated by its recurrence in up to 30% of patients.
An open-label, partially randomized, dose-escalation Phase I trial was performed in two parts. Sixty volunteers aged ≥18 to <65 years were randomized into five treatment groups to receive three immunizations (Day 0, 7, 21) of VLA84 (20μg with Alum, 75μg with or without Alum, 200μg with or without Alum). Eighty-one volunteers aged ≥65 were randomized into four treatment groups (75μg with or without Alum, 200μg with or without Alum) and received four immunizations (Day 0, 7, 28 and 56). All subjects were followed for safety and immunogenicity for six months.
VLA84 was safe and well tolerated. Fifty-one adult volunteers (85%) and 50 elderly (62%) experienced at least one solicited or unsolicited adverse event (AE). Forty-eight adult volunteers (80%) and 40 elderly (49%) experienced related AEs which were mostly mild or moderate. No related serious adverse event and no death occurred. The vaccine induced high antibody titres against Toxin A and Toxin B in both study populations.
VLA84 was safe, well tolerated and highly immunogenic in adult volunteers aged ≥18 to <65 years and elderly volunteers aged ≥65 years. This study is registered at ClinicalTrials.gov under registration number NCT01296386.
艰难梭菌感染(CDI)是抗生素相关性腹泻和结肠炎的主要病因,也是医疗保健相关感染最常见的病原体。在美国,CDI导致约50万例感染,近3万例死亡。尽管对抗生素相关性艰难梭菌腹泻进行了治疗,但仍有高达30%的患者出现疾病复发,使病情复杂化。
一项开放标签、部分随机、剂量递增的I期试验分两部分进行。60名年龄≥18至<65岁的志愿者被随机分为五个治疗组,接受三次VLA84免疫接种(第零天、第7天、第21天)(20μg加明矾、75μg加或不加明矾、200μg加或不加明矾)。81名年龄≥65岁的志愿者被随机分为四个治疗组(75μg加或不加明矾、200μg加或不加明矾),并接受四次免疫接种(第零天、第7天、第28天和第56天)。所有受试者均接受为期六个月的安全性和免疫原性随访。
VLA84安全且耐受性良好。51名成年志愿者(85%)和50名老年志愿者(62%)经历了至少一次预期或非预期不良事件(AE)。48名成年志愿者(80%)和40名老年志愿者(49%)经历了相关AE,大多为轻度或中度。未发生相关严重不良事件,也无死亡病例。该疫苗在两个研究人群中均诱导产生了针对毒素A和毒素B的高抗体滴度。
VLA84在年龄≥18至<65岁的成年志愿者和年龄≥65岁的老年志愿者中安全、耐受性良好且具有高度免疫原性。本研究已在ClinicalTrials.gov注册,注册号为NCT01296386。
