Abstract
Introduction
Influenza is an important cause of morbidity and mortality in Europe. Prevention by annual vaccination is most effective but with yearly vaccine reformulation to match circulating virus strains, vaccine safety must be continuously monitored. The European Medicines Agency published guidance on safety monitoring of influenza vaccines.
Methods
An enhanced safety surveillance study of GSK’s inactivated quadrivalent influenza vaccine (IIV4) was conducted in Belgium, Germany, and Spain in influenza season 2018/19. The objective was to collect adverse event (AE) reports from subjects within 7 days of vaccination. A customized AE reporting card (AERC) with predefined AEs of interest was used to rapidly detect and evaluate potential new safety concerns. Interim results are presented here.
Results
Between week 40 and 52, 1060 vaccinated subjects were enrolled (31.0% Belgium, 26.2% Germany, and 42.7% Spain) covering all ages for which IIV4 is indicated (32.0% aged 6 months–17 years, 33.8% 18–65 years, and 34.2% over 65 years). Pediatric subjects less than 9 years old (n = 139) received two doses. Following dose 1 and dose 2, 98.2% and 100%, respectively, returned the completed AERC recording any AEs. Following dose 1 and dose 2, 454 and 34 subjects, respectively, reported at least one AE (most frequently expected general and injection site symptoms and respiratory symptoms).
Conclusion
All reported AEs were expected as per summary product characteristics (smPC). No safety signals that impact public health or alter the benefit–risk profile of GSK’s IIV4 were identified. Subjects from all vaccinated age groups were enrolled and the use of AERCs allowed rapid monitoring and analysis of reported AEs.
Trial Registration
ClinicalTrials.gov identifier, NCT03688620.
Funding
GlaxoSmithKline Biologicals SA.
Electronic supplementary material
The online version of this article (10.1007/s12325-019-01105-2) contains supplementary material, which is available to authorized users.
Keywords: AlphaRix Tetra, Infectious disease, Influenza, Influsplit Tetra, Fluarix Tetra, Post marketing surveillance, Safety, Vaccination
Introduction
The burden of seasonal influenza in Europe is substantial. A study published by the European Center for Disease Prevention and Control (ECDC) in 2018 ranked influenza as having the highest burden among 31 infectious diseases assessed. Influenza incidence and mortality were high with 5887 cases and 5.89 deaths per 100,000 population. Compared to the other infectious diseases, the burden of influenza ranked second for the age group under 15 years, third among adults (16–64 years), and was by far the highest among older people (over 65 years) [1].
Seasonal epidemics of influenza are caused by circulating influenza A virus subtypes and B virus lineages. Annual vaccination is the most effective approach to preventing influenza and its complications [2]. The influenza virus, however, undergoes frequent genetic and antigenic changes; therefore, each year new vaccines are formulated to match the circulating virus strains, based on recommendations from the World Health Organization (WHO) [3].
GSK’s seasonal inactivated quadrivalent influenza vaccine (IIV4) is indicated for active immunization of adults and children from 6 months of age for the prevention of influenza disease caused by the two influenza A virus subtypes and the two influenza B virus lineages contained in the vaccine.
As seasonal vaccines are typically reformulated annually and introduced in a short time span and to a large number of people, their benefit–risk profile must be routinely monitored and their safety rapidly assessed [4]. The European Medicines Agency (EMA) updated their guidance to vaccine manufacturers in this respect in 2014, no longer recommending small clinical trials for newly formulated vaccines prior to introduction, as these provided limited information on expected efficacy and safety [5]. Instead, they recommend early annual enhanced safety surveillance in one or several European Union member states, where data and systems permit the objective to be met quickly. The main objective is to rapidly detect and act on any new safety signals, i.e., increased frequency or severity of expected reactogenicity (e.g., local, systemic, or allergic events) intrinsic to each vaccine, compared to previous season or clinical trial rates, that could indicate a more serious risk [4].
Following an initial pilot study in the United Kingdom (UK) [6] in influenza season 2015/16, GSK refined an enhanced safety surveillance (ESS) methodology, using customized adverse event reporting cards (AERC). This was then successfully applied in the UK to assess vaccine safety in influenza seasons 2016/17 [7, 8] and 2017/18 (NCT03278067), mostly in adults and older adults because of preferential local recommendations for a live attenuated influenza vaccine (LAIV), except when contraindicated. In both studies, using the AERC increased reporting of EMA-specified adverse events of interest (AEIs) compared with electronic health records which require a medical visit.
The objective of the current ESS study for influenza season 2018/19 was to collect safety data for GSK’s IIV4 in Belgium (AlphaRix Tetra), Germany (Influsplit Tetra), and Spain (Fluarix Tetra), for all age groups for which it is indicated. Of note, the different brand names by country refer to the same medicinal product (IIV4). The primary objective was to estimate the cumulative percentage of subjects reporting AEIs and/or other AEs, using the AERC, within 7 days following vaccination with IIV4. The secondary objectives were to estimate the weekly and cumulative data by age strata (6 months–17 years; 18–65 years; > 65 years), and risk status (at risk/not at risk). Results of the interim analysis showing weekly AEs reported from week 40 to 52 overall and by country are presented here.
Methods
Study Setting and Population
This ESS study was a prospective multicenter study in Belgium, Germany, and Spain of GSK’s IIV4 during the 2018/19 influenza season. Nine healthcare professionals (HCP) (three in each country) aimed to recruit a total of 1000 subjects (aged 18 years or older in Belgium and Germany, and 6 months or older in Spain) who received IIV4. Vaccination must have been performed in routine clinical practice according to local prescribing information, with one dose for subjects previously vaccinated against influenza or aged over 9 years, and two doses (4 weeks apart) for subjects aged under 9 years and not previously vaccinated against influenza [9]. Written informed consent/assent was obtained from subjects or their parents/guardians prior to enrollment. Subjects aged 6 months or older at the time of vaccination with IIV4, who consented and who would, according to investigators, comply with the protocol, were included in the study. Children in care were excluded from the study (i.e., children under the control or protection of an agency, organization, institution, or entity by the courts, the government, or a government body, acting in accordance with powers conferred on them by law or regulation).
The study was conducted between October 1, 2018 and January 4, 2019 with recruitment planned from October 1 to December 31, 2018 for subjects requiring one dose, and from October 1 to December 1, 2018 for subjects requiring two doses. Study follow-up was approximately 8 days for subjects vaccinated with one dose and 36 days for subjects vaccinated with two doses.
Selection of Countries
A feasibility assessment of suitable countries for the conduct of this study was made and suitable research groups and sites were contacted. The study was conducted in Belgium, Germany, and Spain. Despite similar vaccine recommendations in these three countries (primarily targeting older adults and children at risk for annual influenza vaccination), sites in Spain that responded favorably were essentially pediatric sites, while Belgium and Germany have limited vaccine coverage in children. As such, Belgium and Germany only recruited subjects 18 years of age and above (with German participating sites targeting subjects aged 50 years and older). Spain targeted the enrollment of subjects between 6 months and 65 years of age at the time of the vaccination. This study was thus able to capture data on AEs in all age groups with an indication for GSK’s seasonal influenza vaccine, regardless of the target population for vaccination.
Safety Data Collection and Analysis
This study aimed to capture AEs in near real time in order to rapidly estimate the reporting rate of AEIs experienced within days of vaccination. Weekly data reviews and four interim analyses were conducted. The results of the fourth interim analysis are presented here. An AE was defined as any untoward medical occurrence, temporally associated with the use of a medicinal product (whether or not related to the product) or with a study procedure. The HCPs provided each vaccinee or their parent/guardian with a customized AERC to be completed from the day of vaccination and for the following 6 days. The AERC includes predefined categories of AEIs representing events commonly associated with IIV4 s, along with a free text field to report any other AE, and the possibility to indicate that no AE occurred in the 7-day timeframe. Subjects were asked to return the AERC to their HCP at the next scheduled visit or by mail within 2 weeks of vaccination. Practice staff then entered the information in an electronic Case Report Form (eCRF), using a code list provided to each practice to standardize data collection and analysis of AEIs. Details on the AERC and eCRF were previously published by the authors [10]. Reported AEIs were coded using the Medical Dictionary for Regulatory Activities (MedDRA) classification [11].
Statistical Considerations
In the sample size calculations, the probability of observing at least one AE was presented according to several scenarios in which the expected number of vaccinees and true percentage of subjects experiencing an AE were tabulated. Those scenarios were previously reported in the published protocol [10]. Of note, the planned number of study subjects to be enrolled (n = 1000) was expected to enable detection of the very common (≥ 1/10), common (≥ 1/100 to < 1/10), uncommon (≥ 1/1000 to < 1/100) AEIs, and/or other AEs.
Demographic data collected for all subjects, including age, gender, geographic ancestry, and risk status, are presented for the overall study population. The HCP assessed and recorded each subject as at risk/not at risk for influenza-associated morbidity and mortality according to the local recommendations. Of note, in Europe, according to ECDC [12], risk groups should include pregnant women, subjects with chronic conditions (e.g., heart or lung diseases, metabolic or renal disease, chronic liver disease, chronic neurological conditions, or immunodeficiencies), older subjects in long-term care facilities, children aged 6–59 months, and healthcare workers. The interim analysis was conducted on all vaccinated subjects who received the AERC. The number and percentage of vaccinated subjects are presented by country and center, by International Standards Organization (ISO) week) of vaccination, and by age category (6 months–17 years, 18–65 years, over 65 years). The number and percentage of subjects returning their AERC are presented by country/center and for dose 1 and dose 2. The occurrences of AEs are presented by AEI or other AE by Preferred Term (PT) by vaccination week (expected ISO weeks 40–52) using the MedDRA classification for Primary System Organ Class, overall and by country. All analyses were descriptive in nature and did not aim to allow direct comparisons. The extended Clopper–Pearson exact confidence interval (CI) for cluster data was used to compute 95% CI on all estimated percentages, accounting for clustering effect of centers [13].
Compliance with Ethics Guidelines
The study was conducted in accordance with the International Conference on Harmonisation (ICH) Guideline for Good Clinical Practice, Good Epidemiology Practice, Good Pharmacovigilance Practice, or other applicable guidelines, all applicable subject privacy requirements and the guiding principles of the Declaration of Helsinki. The study was designed and conducted in accordance with the ICH Harmonised Tripartite Guideline for clinical investigation of medicinal products in the paediatric population (ICH E11) and all other applicable ethical guidelines. GSK obtained favourable opinion/approval to conduct the study prior to a site initiating the study in that country or has documented that neither a favourable opinion nor an approval to conduct the study was needed. Written informed consent/assent was obtained from subjects or their parents/guardians prior to enrolment. The study received approval from the following ethics committees (ECs), or institutional review boards (IRBs) and regional authorities were consulted consistent with country requirements, namely Commissie Medische Ethiek UZ/KU Leuven (EC) in Belgium (approval received 24 August); Ethik-Kommission der Bayerischen (EC) in Germany (approval received 20 September), and in Spain the PEIBA (IRB and RA combined) for Andalusia (approval received 26 September) and Hospital Vall de Hebron (IRB) and Goli Gurina (RA) for Catalonia (approval received 22 October). GSK posted the study protocol on GSK’s Clinical Study Register (accessible at www.gsk-clinicalstudyregister.com, GSK Study ID 207737) and on the US National Library of Medicine website www.clinicaltrials.gov (NCT03688620).
Results
In total, 1060 vaccinated subjects were included between October 5, 2018 (ISO week 40) and December 31, 2018 (ISO week 52), of which 329 (31.0%) were from Belgium, 278 (26.2%) were from Germany, and 453 (42.7%) were from Spain (Table 1). All subjects were vaccinated with dose 1 and 139 subjects aged less than 9 years in Spain received dose 2. All subjects in the age category 6 months–17 years (n = 339, 32.0%) were from Spain, while 358 subjects (33.8%) aged 18–65 years were from all three countries and 363 subjects (34.2%) aged over 65 years were from Belgium and Germany (Fig. 1). The median age of subjects was 68 years in Belgium and Germany and 6 years in Spain (mean age overall 42.8 years). Overall 51.3% of subjects were female and 98.0% were Caucasian. Subjects assessed as being at risk for influenza-associated morbidity and mortality were distributed as follows: 204 (62.0%) in Belgium, 133 (47.8%) in Germany, and 223 (49.2%) in Spain (Table 2). For those subjects receiving two doses, median age was 3 years, 42.2% were female, 99.3% were Caucasian, and 34.5% were assessed as at risk for influenza-associated morbidity and mortality.
Table 1.
Country | Total vaccinated subjects enrolled, N = 1060 | |||||
---|---|---|---|---|---|---|
Center | N | %a | Age group | N | %a | |
Belgium | 237303 | 129 | 12.2 | 6 months–17 years | 0 | 0 |
237304 | 36 | 3.4 | 18–65 years | 133 | 12.5 | |
237305 | 164 | 15.5 | > 65 years | 196 | 18.5 | |
All | 329 | 31.0 | All | 329 | 31.0 | |
Germany | 237278 | 135 | 12.7 | 6 months–17 years | 0 | 0 |
237279 | 93 | 8.8 | 18–65 years | 111 | 10.5 | |
237280 | 50 | 4.7 | > 65 years | 167 | 15.8 | |
All | 278 | 26.2 | All | 278 | 26.2 | |
Spain | 236682 | 250 | 23.6 | 6 months–17 years | 339 | 32.0 |
236684 | 153 | 14.4 | 18–65 years | 114 | 10.8 | |
237680 | 50 | 4.7 | > 65 years | 0 | 0 | |
All | 453 | 42.7 | All | 453 | 42.7 |
N total number of subjects, n number and % (percentage) of subjects in a given center or age group and country
aDue to the rounding of the percentages to 1 decimal, the total may not equal 100%
Table 2.
Belgium N = 329 | Germany N = 278 | Spain N = 453 | Overall N = 1060 | |||||
---|---|---|---|---|---|---|---|---|
Value or n | % | Value or n | % | Value or n | % | Value or n | % | |
Age (year) at dose 1 vaccination | ||||||||
Median | 68.0 | 68.5 | 6.0 | 48.0 | ||||
Maximum | 91 | 100 | 64 | 100 | ||||
Minimum age (month/year) at dose 1 vaccination | 23 years | 18 years | 6 months | 6 months | ||||
Age category at dose 1 vaccination | ||||||||
6 months–17 years | 0 | 0.0 | 0 | 0.0 | 339 | 74.8 | 339 | 32.0 |
18–65 years | 133 | 40.4 | 111 | 39.9 | 114 | 25.2 | 358 | 33.8 |
> 65 years | 196 | 59.6 | 167 | 60.1 | 0 | 0.0 | 363 | 34.2 |
Gender | ||||||||
Female | 147 | 44.7 | 166 | 59.7 | 231 | 51.0 | 544 | 51.3 |
Male | 182 | 55.3 | 112 | 40.3 | 222 | 49.0 | 516 | 48.7 |
Geographic ancestry | ||||||||
Black or African American | 0 | 0.0 | 2 | 0.7 | 1 | 0.2 | 3 | 0.3 |
Asian—Central/South Asian | 1 | 0.3 | 1 | 0.4 | 1 | 0.2 | 3 | 0.3 |
Asian—East Asian | 4 | 1.2 | 1 | 0.4 | 0 | 0.0 | 5 | 0.5 |
Asian—South East Asian | 2 | 0.6 | 0 | 0.0 | 0 | 0.0 | 2 | 0.2 |
White—Arabic/North African | 1 | 0.3 | 0 | 0.0 | 3 | 0.7 | 4 | 0.4 |
White—Caucasian/European | 321 | 97.6 | 274 | 98.6 | 444 | 98.0 | 1039 | 98.0 |
Other | 0 | 0.0 | 0 | 0.0 | 4 | 0.9 | 4 | 0.4 |
Risk status: influenza-associated morbidity and mortalitya | ||||||||
At risk | 204 | 62.0 | 133 | 47.8 | 223 | 49.2 | 560 | 52.8 |
Not at risk | 125 | 38.0 | 145 | 52.2 | 230 | 50.8 | 500 | 47.2 |
ISO International Standards Organization, N number of subjects vaccinated, n number and % (percentage) of vaccinated subjects in a given category
aAssessed by the HCP based on his/her judgment and experience
The majority of subjects aged 6 months–17 years received dose 1 in ISO weeks 42–45 in Spain. Most adults (18–65 years) in Belgium and Germany were vaccinated earlier (in ISO week 42 for Belgium and ISO weeks 40–42 for Germany) while those in Spain were mostly vaccinated later (ISO weeks 45–46). Among the older adults (> 65 years), most in Germany were vaccinated early (ISO weeks 40–42) while those in Belgium were typically vaccinated later (ISO weeks 43–46) (Fig. 1).
Following each vaccination, all subjects received an AERC to complete and return. Overall, by January 14, 2019, 98.2% of AERCs were returned (94.8% in Belgium, 99.6% in Germany, and 99.8% in Spain) for dose 1. For dose 2 in Spain, 100% of AERCs were returned (Table 3).
Table 3.
Country | Center | Dose 1 | Dose 2 | ||||
---|---|---|---|---|---|---|---|
N | AERC returned | N | AERC returned | ||||
n | % | n | % | ||||
Belgium | 237303 | 129 | 112 | 86.8 | – | – | – |
237304 | 36 | 36 | 100 | – | – | – | |
237305 | 164 | 164 | 100 | – | – | – | |
All | 329 | 312 | 94.8 | – | – | – | |
Germany | 237278 | 135 | 134 | 99.3 | – | – | – |
237279 | 93 | 93 | 100 | – | – | – | |
237280 | 50 | 50 | 100 | – | – | – | |
All | 278 | 277 | 99.6 | – | – | – | |
Spain | 236682 | 250 | 250 | 100 | 116 | 116 | 100 |
236684 | 153 | 152 | 99.3 | 4 | 4 | 100 | |
237680 | 50 | 50 | 100 | 19 | 19 | 100 | |
All | 453 | 452 | 99.8 | 139 | 139 | 100 | |
Overall | All | 1060 | 1041 | 98.2 | 139 | 139 | 100 |
AERC adverse event reporting card, N number of subjects vaccinated who received the AERC, n number and % (percentage) of subjects vaccinated who returned the AERC as specified
The percentage of subjects reporting AEIs and other AEs (classed according to MedDRA Primary System Organ Class [PSOC] and Preferred Term [PT]) is presented for all countries following dose 1 (Table 4) and dose 2 (Table 5).
Table 4.
MedDRA primary system organ class (CODE) | N = 1060 | |
---|---|---|
Preferred term (code) | n | % |
Any | 454 | 42.8 |
Any general disorders and administration site conditions (10018065) | 301 | 28.4 |
Injection site pain (10022086)* | 185 | 17.5 |
Injection site swelling (10053425)* | 80 | 7.5 |
Fatigue (10016256)* | 69 | 6.5 |
Injection site erythema (10022061)* | 56 | 5.3 |
Pyrexia (10037660)* | 33 | 3.1 |
Chills (10008531)* | 25 | 2.4 |
Injection site pruritus (10022093) | 4 | 0.4 |
Face edema (10016029)* | 2 | 0.2 |
Influenza-like illness (10022004); mucous membrane disorder (10028133); peripheral swelling (10048959) | 2 each | 0.2 each |
Discomfort (10013082); feeling cold (10016326); feeling hot (10016334); injection site hematoma (10022066); injection site reaction (10022095); injection site warmth (10022112); malaise (10025482) | 1 each | 0.1 each |
Any respiratory, thoracic, and mediastinal disorders (10038738) | 184 | 17.4 |
Rhinorrhea (10039101)* | 91 | 8.6 |
Cough (10011224)* | 71 | 6.7 |
Nasal congestion (10028735)* | 56 | 5.3 |
Oropharyngeal pain (10068319)* | 49 | 4.6 |
Dysphonia (10013952)* | 23 | 2.2 |
Epistaxis (10015090)* | 9 | 0.8 |
Wheezing (10047924)* | 6 | 0.6 |
Dyspnea (10013968); sneezing (10041232) | 3 each | 0.3 each |
Dry throat (10013789); increased upper airway secretion (10062717); pharyngeal inflammation (10065716); throat clearing (10080125) | 1 each | 0.1 each |
Any musculoskeletal and connective tissue disorders (10028395) | 95 | 9.0 |
Myalgia (10028411)* | 71 | 6.7 |
Arthropathy (10003285)* | 32 | 3.0 |
Pain in extremity (10033425) | 3 | 0.3 |
Rheumatic disorder (10072736) | 2 | 0.2 |
Limb discomfort (10061224); muscle spasms (10028334); musculoskeletal pain (10028391); synovial cyst (10042858) | 1 each | 0.1 each |
Any nervous system disorders (10029205) | 85 | 8.0 |
Headache (10019211)* | 78 | 7.4 |
Dizziness (10013573) | 4 | 0.4 |
Aphonia (10002953); poor quality sleep (10062519); somnolence (10041349); tremor (10044565) | 1 each | 0.1 each |
Febrile convulsion (10016284)* | 0 | 0.0 |
Any gastrointestinal disorders (10017947) | 67 | 6.3 |
Diarrhea (10012735)* | 32 | 3.0 |
Nausea (10028813)* | 32 | 3.0 |
Vomiting (10047700)* | 19 | 1.8 |
Abdominal pain (10000081) | 3 | 0.3 |
Gingival bleeding (10018276); lip swelling (10024570); stomatitis (10042128); tongue discomfort (10077855) | 1 each | 0.1 each |
Any infections and infestations (10021881) | 66 | 6.2 |
Conjunctivitis (10010741)* | 36 | 3.4 |
Rhinitis (10039083)* | 30 | 2.8 |
Nasopharyngitis (10028810) | 3 | 0.3 |
Bronchitis (10006451); ear infection (10014011); herpes simplex (10019948); hordeolum (10020377); laryngitis (10023874); oral herpes (10067152); upper respiratory tract infection (10046306) | 1 each | 0.1 each |
Any metabolism and nutrition disorders (10027433) | 32 | 3.0 |
Decreased appetite (10061428)* | 32 | 3.0 |
Any psychiatric disorders (10037175) | 19 | 1.8 |
Irritability (10022998)* | 18 | 1.7 |
Insomnia (10022437); mood swings (10027951); sleep disorder (10040984) | 1 each | 0.1 each |
Any skin and subcutaneous tissue disorders (10040785) | 17 | 1.6 |
Pruritus (10037087) | 8 | 0.8 |
Rash (10037844)* | 7 | 0.7 |
Erythema (10015150) | 2 | 0.2 |
Hyperhidrosis (10020642); pruritus generalized (10052576) | 1 each | 0.1 each |
Rash generalized (10037858)* | 0 | 0.0 |
Any ear and labyrinth disorders (10013993) | 7 | 0.7 |
Ear pain (10014020); vertigo (10047340) | 2 each | 0.2 each |
Ear hemorrhage (10014009); ear pruritus (10052138); tinnitus (10043882) | 1 each | 0.1 each |
Any immune system disorders (10021428) | 6 | 0.6 |
Hypersensitivity (10020751)* | 6 | 0.6 |
Anaphylactic reaction (10002198)* | 0 | 0.0 |
Any investigations (10022891) | 4 | 0.4 |
Heart rate increased (10019303) | 4 | 0.4 |
Any eye disorders (10015919) | 3 | 0.3 |
Eye pruritus (10052140); lacrimation increased (10023644); swelling of eyelid (10042690) | 1 each | 0.1 each |
Any injury, poisoning, and procedural complications (10022117) | 1 | 0.1 |
Muscle strain (10050031) | 1 | 0.1 |
Any cardiac disorders (10007541) | 1 | 0.1 |
Tachycardia (10043071) | 1 | 0.1 |
AE adverse event, AEI adverse event of interest, AERC adverse event reporting card, MedDRA Medical Dictionary for Regulatory Activities [11], N total number of subjects, n number of subjects in category
*AEI
Table 5.
MedDRA primary system organ class (CODE) | N = 139 | |
---|---|---|
Preferred term (code) | n | % |
Any | 34 | 24.5 |
Any respiratory, thoracic, and mediastinal disorders (10038738) | 21 | 15.1 |
Cough (10011224)* | 12 | 8.6 |
Rhinorrhea (10039101)* | 9 | 6.5 |
Nasal congestion (10028735)* | 7 | 5.0 |
Dysphonia (10013952)* | 3 | 2.2 |
Wheezing (10047924)* | 2 | 1.4 |
Epistaxis (10015090)* | 1 | 0.7 |
Sneezing (10041232) | 1 | 0.7 |
Oropharyngeal pain (10068319)* | 0 | 0.0 |
Any general disorders and administration site conditions (10018065) | 11 | 7.9 |
Injection site pain (10022086)* | 7 | 5.0 |
Pyrexia (10037660)* | 6 | 4.3 |
Chills (10008531)* | 0 | 0.0 |
Face edema (10016029)* | 0 | 0.0 |
Fatigue (10016256)* | 0 | 0.0 |
Injection site erythema (10022061)* | 0 | 0.0 |
Injection site swelling (10053425)* | 0 | 0.0 |
Any infections and infestations (10021881) | 5 | 3.6 |
Conjunctivitis (10010741)* | 4 | 2.9 |
Rhinitis (10039083)* | 1 | 0.7 |
Any gastrointestinal disorders (10017947) | 4 | 2.9 |
Diarrhea (10012735)* | 2 | 1.4 |
Vomiting (10047700)* | 1 | 0.7 |
Abdominal pain (10000081) | 1 | 0.7 |
Nausea (10028813)* | 0 | 0.0 |
Any metabolism and nutrition disorders (10027433) | 4 | 2.9 |
Decreased appetite (10061428)* | 4 | 2.9 |
Any psychiatric disorders (10037175) | 4 | 2.9 |
Irritability (10022998)* | 4 | 2.9 |
Any eye disorders (10015919) | 2 | 1.4 |
Eye pruritus (10052140) | 2 | 1.4 |
Any musculoskeletal and connective tissue disorders (10028395) | 1 | 0.7 |
Myalgia (10028411)* | 1 | 0.7 |
Arthropathy (10003285)* | 0 | 0.0 |
Any skin and subcutaneous tissue disorders (10040785) | 1 | 0.7 |
Rash (10037844)* | 1 | 0.7 |
Rash generalized (10037858)* | 0 | 0.0 |
Any immune system disorders (10021428) | 0 | 0.0 |
Anaphylactic reaction (10002198)* | 0 | 0.0 |
Hypersensitivity (10020751)* | 0 | 0.0 |
Any nervous system disorders (10029205) | 0 | 0.0 |
Febrile convulsion (10016284)* | 0 | 0.0 |
Headache (10019211)* | 0 | 0.0 |
AE adverse event, AEI adverse event of interest, AERC adverse event reporting card, MedDRA Medical Dictionary for Regulatory Activities [11], N total number of subjects, n number of subjects in category
*AEI
Overall, among the 1060 vaccinated subjects, 454 subjects (42.8%) reported at least one AE after dose 1. The most frequently reported AEs were on the predefined list of AEIs, i.e., injection site pain (17.5%), rhinorrhea (8.6%), injection site swelling (7.5%), headache (7.4%), myalgia (6.7%), cough (6.7%), fatigue (6.5%), injection site erythema (5.3%), nasal congestion (5.3%), and oropharyngeal pain (4.6%). Some predefined AEIs were not reported, i.e., there were no cases of anaphylaxis, generalized rash, febrile convulsion, Bell’s palsy, or Guillain–Barré syndrome. Other AEIs were less frequent, reported in 0.2–3.4% of subjects. Regarding AEs not on the predefined list, the most frequently reported was pruritus (0.8%), while other AEs were reported for 0.1–0.4% of subjects. The most frequently reported MedDRA PSOC of AEs were general disorders and administration site conditions (n = 301, 28.4%), followed by respiratory, thoracic ,and mediastinal disorders (n = 184, 17.4%), musculoskeletal and connective tissue disorders (n = 95, 9.0%), nervous system disorders (including headache) (n = 85, 8.0%), gastrointestinal disorders (n = 67, 6.3%) ,and infections and infestations (n = 66, 6.2%). The remaining classes of AEs were reported by 3% or fewer subjects (Table 4).
The overall frequency of AEs reported after dose 1 was similar (i.e., 41.9% in Belgium, 36.7% in Germany, and 47.2% in Spain), and the ranking and frequencies of the most common classes of AEs were mostly of similar magnitude: general disorders reported by 26.7–30.0% of subjects, respiratory disorders by 11.5–23.0%, musculoskeletal disorders by 8.3–10.3%, nervous system disorders (including headache) by 7.9–8.2%, gastrointestinal disorders by 5.0–6.8%, and infections by 4.6–7.9%. In Spain, metabolism disorders (i.e., decreased appetite) were also reported by 5.3% of subjects.
In Spain, among the 139 pediatric subjects who received dose 2, 34 subjects reported at least one AE. The most frequently reported AEs were on the predefined list of AEIs and were classed as respiratory, thoracic, and mediastinal disorders (n = 21, 15.1%) of which cough (8.6%), rhinorrhea (6.5%), and nasal congestion (5.0%) were most frequent. The next most frequently reported AEIs were general disorders and administration site conditions (n = 11, 7.9%) of which injection site pain (5.0%) and pyrexia (4.3%) were most frequent. Other AEIs were reported by 0.7–2.9% of subjects. There were no reports of the following AEIs: headache, febrile convulsion, anaphylaxis, hypersensitivity, generalized rash, arthropathy, nausea, injection site swelling or erythema, fatigue, chills, face edema, oropharyngeal pain, Bell’s palsy, or Guillain–Barré syndrome. AEs not on the predefined list were reported by 0.7–1.4% of subjects (i.e., one case each of sneezing and abdominal pain and two cases of eye pruritus) (Table 5).
In addition, during the study period, according to HCPs judgement, no serious AEs deemed to be related to GSK’s IIV4 were reported within 7 days post vaccination.
In the electronic supplementary material, the percentage of subjects with AEs by ISO week following dose 1 and dose 2 is presented overall and by country. See Tables S1–S5 in the electronic supplementary material for details.
Discussion
At the interim analysis in this study, 100% of AERCs were returned for two out of three centers in each country, while the return rate was 86.8–99.3% for the remaining centers for dose 1. For dose 2, 100% of AERCs were returned. Following dose 1, interim results showed that 454 subjects reported at least one AE within 7 days of vaccination among the 1060 subjects. The most frequently reported were on the predefined list of AEIs, i.e., local injection site reactions and general symptoms (headache, fatigue), respiratory symptoms (rhinorrhea, cough, nasal congestion, oropharyngeal pain), and myalgia. These AEIs were expected events commonly observed after vaccination with an IIV4 [14].
Ongoing reviews of raw data during the study period and the interim analyses did not detect any safety signals that could affect public health or could alter the benefit–risk profile of GSK’s IIV4.
The methodology used for data collection and analysis (i.e., customized AERC completed by subjects and coded into eCRFs by practice staff using a MedDRA-based coding list) also appears to have been successful and a promising approach, with a return rate for AERCs that was in the same range or above the return rate observed in active surveillance. There are two possible explanations for the high return rate: firstly, feedback following similar studies in the UK has revealed a growing interest from patients to participate actively in their health follow-up; and secondly, the study included a planned visit following vaccination, to encourage continued subject participation (see protocol [10]). In Italy, active surveillance 7 days after influenza vaccination involving a follow-up telephone interview or web-based platform resulted in a 97% response rate overall [15]. In the Netherlands, a web-based questionnaire had response rates of 90.7% at day 5, 84.5% at day 15, and 78.4% at day 30 after influenza vaccination [16].
This ESS of GSK’s IIV4 covered all age groups for which the vaccine is indicated. This was achieved through a combination of data from three European countries: Spain, where pediatric subjects were enrolled (from 6 months of age), as well as Germany and Belgium, all of which use IIV4 in adults and older adults. The distribution of subjects across countries and across age categories was generally balanced. The target number of patients was reached in the 3-month recruitment period, with sufficient data collected in a relatively short period of time, as the majority of subjects were vaccinated and enrolled within a 4-week timeframe. Data were also reviewed on an ongoing basis in near real time owing to the electronic application and data collection methods used.
A recent review summarizes several other initiatives conducted so far to address the EMA requirement for enhanced safety surveillance of seasonal influenza vaccines, and illustrates a diverse range of approaches used in Europe (e.g., patient diaries, patient records, interviews) with their challenges. Several studies reported difficulties with the recruitment of pediatric participants or with achieving high response rates [17].
A key strength of this study was the inclusion of a large and diverse group of subjects of all ages for which IIV4 is indicated, and from participating countries with different vaccination practices. Nevertheless, the relatively low number of subjects included did not allow investigation of potential disparities, across age groups notably, which deserves further attention in the future. The study procedures and prospective data collection proved to be successful, given the high return rate of AERCs. The use of an electronic application to collect standardized data (eCRFs using the coded AEI list) simplified data extraction, cleaning, and analysis to facilitate near-real-time assessment of the safety data, and will allow for future comparisons. The main limitations of this observational study were the absence of formal baseline rates for comparison (although final results can be discussed in light of the expected AE rates from clinical trials reported in the smPC), the limited timeframe for AE detection which is not adequate to fully capture AEs with a longer risk period, and that the enrollment period was dependent on the timing of vaccination campaigns in participating countries. Enrollment, thus, could not begin before mid to end October at most participating centers. This was, however, mitigated by a fast recruitment period, condensed into approximately 4 weeks. Given the small number of participating centers, the participants (mainly white-Caucasian) may not be representative of all inhabitants in these countries. Furthermore, the sample size was not large enough to allow for the assessment of rare AEs; however, on the basis of the EMA guidance, this was not an objective of the study.
Conclusion
Importantly, this interim analysis did not show any safety signals for GSK’s IIV4 in the 2018/19 influenza season that could impact public health or the known safety profile of the vaccine. Further analyses will describe the reported AEs in more detail and confirm the current safety findings. This multi-country study and the proposed ESS methodology were successful in rapidly providing safety data from subjects of all ages for whom IIV4 is indicated. It offered a suitable approach for the continuous monitoring of seasonal influenza vaccines, overcoming the underreporting frequently observed with passive initiatives.
Electronic supplementary material
Below is the link to the electronic supplementary material.
Acknowledgements
The authors thank the participating patients, the medical staff who contributed to study implementation, and the clinical practices that allowed pseudonymised data to be extracted from their general practice CMR system. In addition, the authors thank the GSK’s clinical operational teams for their continuous support who ensured a successful study conduct. The authors also thank Jacqueline Miller, Dominique Rosillon, Stephanie Gilon, Alexander Schmidt, Katie Smith, Elvira Zandman Van Dijk, Harish Dasari, Christiane Klein, Lode Godderis, Stephane Vanden Bemden, Hugo Loos, and Xavier Martinez Gomez for their contribution to this study/publication.
AlphaRix Tetra, Influsplit Tetra, and Fluarix Tetra are trademarks of the GSK group of companies.
Funding
GlaxoSmithKline Biologicals SA was the funding source and was involved in all stages of the study. GlaxoSmithKline Biologicals SA also funded the Rapid Service and Open Access Fees.
Medical Writing, Editorial and Other Assistance
The authors thank Business & Decision Life Sciences platform for editorial assistance and manuscript coordination, on behalf of GSK. Kavi Littlewood provided writing support, and Bruno Dumont coordinated manuscript development and editorial support.
Authorship
All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.
Disclosures
Vishvesh Shende declares he is employed by VPN Consultancy Limited working on behalf of the GSK group of companies. Anne Yeakey is employed by the GSK group of companies and hold shares in the GSK group of companies. Gael Dos Santos is employed by the GSK group of companies and hold shares in the GSK group of companies. Silvia Damaso is employed by the GSK group of companies and hold shares in the GSK group of companies.
Compliance with Ethics Guidelines
The study was conducted in accordance with the International Conference on Harmonisation (ICH) Guideline for Good Clinical Practice, Good Epidemiology Practice, Good Pharmacovigilance Practice, or other applicable guidelines, all applicable subject privacy requirements and the guiding principles of the Declaration of Helsinki. The study was designed and conducted in accordance with the ICH Harmonised Tripartite Guideline for clinical investigation of medicinal products in the paediatric population (ICH E11) and all other applicable ethical guidelines. GSK obtained favourable opinion/approval to conduct the study prior to a site initiating the study in that country or has documented that neither a favourable opinion nor an approval to conduct the study was needed. Written informed consent/assent was obtained from subjects or their parents/guardians prior to enrolment. The study received approval from the following ethics committees (ECs), or institutional review boards (IRBs) and regional authorities were consulted consistent with country requirements, namely Commissie Medische Ethiek UZ/KU Leuven (EC) in Belgium (approval received 24 August); Ethik-Kommission der Bayerischen (EC) in Germany (approval received 20 September), and in Spain the PEIBA (IRB and RA combined) for Andalusia (approval received 26 September) and Hospital Vall de Hebron (IRB) and Goli Gurina (RA) for Catalonia (approval received 22 October). GSK posted the study protocol on GSK’s Clinical Study Register (accessible at www.gsk-clinicalstudyregister.com, GSK Study ID 207737) and on the US National Library of Medicine website www.clinicaltrials.gov (NCT03688620).
Data Availability
To request access to patient-level data and documents for this study, please submit an enquiry via www.clinicalstudydatarequest.com.
Footnotes
Enhanced Digital Features
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Associated Data
This section collects any data citations, data availability statements, or supplementary materials included in this article.
Supplementary Materials
Data Availability Statement
To request access to patient-level data and documents for this study, please submit an enquiry via www.clinicalstudydatarequest.com.