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. 2019 Jan 10;17:9. doi: 10.1186/s12916-018-1239-8

The impact of repeated vaccination on influenza vaccine effectiveness: a systematic review and meta-analysis

Lauren C Ramsay 1,2, Sarah A Buchan 1,2, Robert G Stirling 2,3, Benjamin J Cowling 4, Shuo Feng 4, Jeffrey C Kwong 1,2,5,6,7, Bryna F Warshawsky 1,8,
PMCID: PMC6327561  PMID: 30626399

Abstract

Background

Conflicting results regarding the impact of repeated vaccination on influenza vaccine effectiveness (VE) may cause confusion regarding the benefits of receiving the current season’s vaccine.

Methods

We systematically searched MEDLINE, Embase, PubMed, and Cumulative Index to Nursing and Allied Health Literature from database inception to August 17, 2016, for observational studies published in English that reported VE against laboratory-confirmed influenza for the following four vaccination groups: current season only, prior season only, both seasons, and neither season. We pooled differences in VE (∆VE) between vaccination groups by influenza season and type/subtype using a random-effects model. The study protocol is registered with PROSPERO (registration number: CRD42016037241).

Results

We identified 3435 unique articles, reviewed the full text of 634, and included 20 for meta-analysis. Compared to prior season vaccination only, vaccination in both seasons was associated with greater protection against influenza H1N1 (∆VE = 25%; 95% CI 14%, 35%) and B (∆VE = 18%; 95% CI 3%, 33%), but not H3N2 (∆VE = 7%; 95% CI – 7%, 21%). Compared to no vaccination for either season, individuals who received the current season’s vaccine had greater protection against H1N1 (∆VE = 62%; 95% CI 51%, 70%), H3N2 (∆VE = 45%; 95% CI 35%, 53%), and B (∆VE = 64%; 95% CI 57%, 71%). We observed no differences in VE between vaccination in both seasons and the current season only for H1N1 (∆VE = 3%; 95% CI – 8%, 13%), but less protection against influenza H3N2 (∆VE = − 20%; 95% CI – 36%, − 4%), and B (∆VE = − 11%; 95% CI – 20%, − 2%).

Conclusions

Our results support current season vaccination regardless of prior season vaccination because VE for vaccination in the current season only is higher compared to no vaccination in either season for all types/subtypes, and for H1N1 and influenza B, vaccination in both seasons provides better VE than vaccination in the prior season only. Although VE was lower against H3N2 and B for individuals vaccinated in both seasons compared to those vaccinated in the current season only, it should be noted that past vaccination history cannot be altered and this comparison disregards susceptibility to influenza during the prior season among those vaccinated in the current season only. In addition, our results for H3N2 were particularly influenced by the 2014–2015 influenza season and the impact of repeated vaccination for all types/subtypes may vary from season to season. It is important that future VE studies include vaccination history over multiple seasons to evaluate repeated vaccination in more detail.

Electronic supplementary material

The online version of this article (10.1186/s12916-018-1239-8) contains supplementary material, which is available to authorized users.

Keywords: Influenza, Vaccine effectiveness, Repeated vaccination

Background

Seasonal influenza vaccination is the predominant strategy for preventing influenza-related morbidity and mortality. Annual vaccination is recommended because of waning immunity and because influenza strains undergo antigenic drift, necessitating reviewing and, in most seasons, changing the vaccine to better match the upcoming season’s strains [1]. Because of the frequently changing vaccine, influenza vaccine effectiveness (VE) is assessed annually.

With increasing numbers of people being immunized against influenza annually, the impact of repeated vaccination has gained significant interest. Of particular interest are older adults (65 years and older), who tend to have more comorbidities as they age, as both age and co-morbidities increase their risk of influenza-associated complications [2]. If repeated vaccination negatively impacts current VE, then having been repeatedly vaccinated in earlier years may be detrimental to the protection of older adults when they need it most. Studies from the 1970s and 1980s found inconsistent results regarding the impact of repeated vaccination [3, 4]. In 1999, a systematic review and meta-analysis of field studies, trials, and serologic studies found no evidence of negative impacts of repeated vaccination [5]. More recently, some studies have found VE to be reduced in those who received repeated prior influenza vaccinations [68].

Since most VE studies now report estimates taking into account vaccination status for both current and prior seasons, we sought to evaluate the impact of repeated vaccination on VE through a systematic review and meta-analysis. We aimed to assess the impact of repeated vaccination to provide evidence to support patient and clinician decision-making about receiving the current season’s influenza vaccine. We considered two patient-relevant scenarios: (1) for someone who received last season’s vaccine, should he/she also receive this season’s vaccine? (vaccination in both seasons versus prior season only); and (2) for someone who did not receive last season’s vaccine, should he/she receive this season’s vaccine? (vaccination in current season only versus neither season). We also considered a policy-relevant scenario, comparing VE for vaccination in both seasons versus the current season only. This latter scenario is not relevant to patients because they cannot alter their vaccination history; however, the findings may influence policy decisions regarding whether or not to offer annual vaccination to the entire population if there was evidence suggesting that repeated vaccination could negatively impact future VE.

Methods

Search strategy and selection criteria

We searched MEDLINE, Embase, PubMed, and Cumulative Index to Nursing and Allied Health Literature (CINAHL) databases from inception to August 17, 2016. We developed a unique search strategy for each database with the assistance of a scientific librarian; across all databases, search terms included “influenza,” “immunization,” “vaccine,” and “effectiveness,” and articles were restricted to those published in English (Additional file 1). Two reviewers (SB, LR) independently screened titles and abstracts, and hand-searched the references of the included articles.

Eligible studies used observational study designs (e.g., prospective cohort, test-negative case-control) and reported VE against medically attended, laboratory-confirmed influenza for four mutually exclusive vaccination groups: current season only, prior season only, both current and prior seasons, and neither season (reference group). Prior season vaccination referred primarily to vaccination status in the year immediately prior to the season being examined. Studies with other definitions of prior season (e.g., any dose in the prior two seasons) were excluded from the meta-analysis, but were described in a qualitative synthesis. We excluded interim VE reports that were superseded by end-of-season reports, and conference abstracts and proceedings. We followed the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines for reporting results [9].

Risk of bias assessment

We used the Newcastle-Ottawa scale (NOS) to assess the risk of bias of included case-control and cohort studies [10]. Two reviewers (SB, LR) independently evaluated the quality of each study based on the domains of selection, comparability, and either exposure (for case-control studies) or outcome (for cohort studies). For studies using the test-negative design, we determined whether calendar time had been included in the adjusted analyses [11]. Studies were categorized as being at low, moderate, or high risk of bias if they were missing ≤ 1 item, 2–3 items, or > 3 items on the NOS, respectively [12]. Any disagreements between the two reviewers were resolved by consensus.

Data analysis

Two reviewers (SB, LR) abstracted the data using a structured electronic data extraction form, extracting study characteristics (e.g., study design, recruitment setting, case definition) and VE estimates for the four vaccination groups, with discrepancies adjudicated by consensus. Whenever possible, we extracted VE reports by influenza type/subtype and age group provided in the articles and only included the most specific results reported (e.g., by age group or influenza type/subtype) in the meta-analysis. Because specific lineage information for influenza B was often unavailable, we used overall estimates for influenza B.

For each study included in the meta-analysis, VE estimates for current season only, prior season only, and both current and prior seasons were assessed against the reference group who were not vaccinated in either season. In the present study, VE estimates from each study were compared for those vaccinated in both the current and prior seasons to those vaccinated in the prior season only and to those vaccinated in the current season only by subtracting the VE estimates. The absolute differences in VE (ΔVE) was stratified by influenza type/subtype and season and calculated as follows: (a) vaccinated in both seasons compared to the prior season only (ΔVE = VEboth − VEprior only) and (b) vaccinated in both seasons compared to the current season only (ΔVE = VEboth − VEcurrent only). In both of the above scenarios, ΔVE greater than zero implies a higher VE estimate when vaccinated in both seasons than in either the current or the prior season only. We also assessed the VE of those vaccinated in the current season only compared to those vaccinated in neither season (pooled VEcurrent only).

We calculated confidence intervals for ΔVE by bootstrapping using 1000 samples [13]. Similar to previous work [14], we took 1000 samples from VEcurrent only, VEprior only, and VEboth. We then estimated 1000 measures of ΔVE for both ΔVE = VEboth − VEcurrent only and ΔVE = VEboth − VEprior only; the 2.5% and 97.5% percentiles for ΔVE were computed as the confidence intervals. We used a random effects model to pool ΔVE estimates to compare the overall difference between vaccination in both seasons with vaccination in either the prior season only or the current season only. To compare VE for those vaccinated in the current season versus those vaccinated in neither season, we used a random effects model to pool the log odds ratio of the current season only VE estimates and converted the final pooled estimate back to a measure of VE. Statistical heterogeneity was assessed using the I2 statistic and Cochran’s Q test. Meta-analyses were performed in MetaXL (Version 2.2, EpiGear International Ltd., Queensland, Australia) with bootstrapping procedures and figures produced in R (Version 3.3.1, R Foundation for Statistical Computing, Vienna, Austria).

Results

The results presented below have been corrected from our previously published review on this topic. The previous article included one study that did not meet the inclusion criteria, omitted one estimate from an included study, and included two estimates from populations that were already included in other estimates (i.e., estimates from a subset of a population that were also captured in other included estimates).

We identified 3435 unique articles from the database searches (Fig. 1). After screening titles and abstracts, we selected 634 articles for full-text review. Of these, 26 studies met the inclusion criteria for the qualitative synthesis, and 20 were included in the meta-analysis [68, 1537]. We observed excellent agreement between reviewers for the title and abstract screen (kappa, Ƙ = 0.94) and for the full-text review (Ƙ = 0.98). No additional studies were identified from hand-searching references. One study was excluded from the qualitative synthesis and meta-analysis because, while it included persons with laboratory-confirmed influenza in the vaccination groups of interest, the study provided VE estimates only for severe or fatal influenza outcomes rather than for any laboratory-confirmed influenza [38]. We excluded six studies from the meta-analysis but included them in the qualitative synthesis: four studies because they only provided VE estimates for any influenza rather than by influenza type/subtype [15, 23, 31, 32], and two studies because they provided VE estimates for any influenza and “prior season vaccination” was not restricted to the immediate year prior to the study season [16, 26].

Fig. 1.

Fig. 1

PRISMA flow diagram of study selection

The 26 included studies captured influenza seasons between 2004–2005 and 2014–2015, with most reporting estimates for the 2010–2011 to 2014–2015 seasons (Table 1). One study was from the Southern hemisphere [32], one study was restricted to pregnant women [35], and two studies were in pediatric populations [17, 34]. Most studies featured outpatient data, but two studies used solely inpatient data [25, 37], and two studies used data from both settings [15, 16]. All studies used reverse-transcriptase polymerase chain reaction (RT-PCR) testing to confirm influenza infection.

Table 1.

Study characteristics of articles included in the meta-analysis and/or qualitative synthesis

Author, publication year Country Study design Current season Prior season Influenza type Age group
Jimenez-Jorge et al., 2012 [19] Spain Test-negative case-control 2010–2011 2009–2010 H1N1 All ages
Martinez-Baz et al., 2013 [20] Spain Test-negative case-control 2010–2011 2009–2010 H1N1 All ages
Skowronski et al., 2012 [28] Canada Test-negative case-control 2010–2011 2009–2010 H1N1 All ages
Syrjanen et al., 2014 [33] Finland Cohort 2010–2011 2009–2010 H1N1 18–75 years
Fu et al., 2015 [17] China Case-control 2012–2013 2011–2012 H1N1 (a) 20–35 months, 1 current dose; (b) 20–35 months, 2 current doses; (c) 3–6 years
Gaglani et al., 2016 [18] USA Test-negative case-control 2013–2014 2009–2010 to 2012–2013 H1N1 ≥ 9 years
Ohmit et al., 2016 [22] USA Prospective cohort study 2013–2014 2012–2013 H1N1 (a) 9 and older; (b) under 9 years
Thompson et al., 2014b [35] USA Case-control 2010–2011 and 2011–2012 2009–2010 and 2010–2011 H1N1, H3N2, B Mean age 30 years
Skowronski et al., 2014b [29] Canada Test-negative case-control 2011–2012 2010–2011 H1N1, H3N2, B ≥ 2 years
Rondy et al., 2015 [25] France, Italy, Lithuania, Spain Test-negative case-control 2012–2013 2011–2012 H1N1, H3N2, B ≥ 18 years
Skowronski et al., 2014a [27] Canada Test-negative case-control 2012–2013 2011–2012 H1N1, H3N2, B ≥ 2 years
Valenciano et al., 2016 [36] Germany, Hungary, Ireland, Italy, Poland, Portugal, Romania, Spain Test-negative case-control 2014–2015 2013–2014 H1N1, H3N2, B All ages
Pebody et al., 2013 [24] UK Test-negative case-control 2010–2011 2009–2010 H1N1, B All ages
Skowronski et al., 2015 [30] Canada Test-negative case-control 2013–2014 2012–2013 H1N1, B ≥ 2 years
McLean et al., 2014 [6] USA Test-negative case-control 2004–2005 to 2012–2013 Variable H3N2, B (a) 9 to 49; (b) 50 and older
McLean et al., 2015 [21] USA Test-negative case-control 2012–2013 2011–2012 H3N2, B (a) 9 to 17; (b) 18 to 49; (c) 50 to 64; (d) 65 and older
Thompson et al., 2016 [34] USA Test-negative case-control 2011–2012 and 2012–2013 2010–2011 and 2011–2012 H3N2, B 2–8 years, 1 dose prior season
Skowronski et al., 2016 [7] Canada Test-negative case-control 2014–2015 2013–2014 H3N2, B ≥ 2 years
Simpson et al., 2015a[26] Scotland Test-negative case-control 2008–2009 9 prior seasons All influenza All ages
Castilla et al., 2011a [15] Spain Nested test-negative case- control 2010–2011 2009–2010 All influenza All ages
Ohmit et al., 2014 [8] USA Test-negative case-control 2011–2012 2010–2011 H3N2 ≥ 9 years
Ohmit et al., 2015a [23] USA Prospective cohort study 2012–2013 2011–2012 All influenza All ages
Smithgall et al., 2016a [31] USA Surveillance 2013–2014 2012–2013 All influenza All ages
Castilla et al., 2016a [16] Spain Test-negative case-control 2014–2015 2013–2014 and 2012–2013 All influenza All ages
Sullivan and Kelly, 2013a [32] Australia Re-analysis (a) Southern Hemisphere 2011; (b) Southern Hemisphere 2012 Southern Hemisphere 2010 and 2011 All influenza All ages
Petrie et al., 2016 [37] USA Test-negative case-control 2014–2015 2013–2014 H3N2 ≥ 18 years

aStudy not included in meta-analysis

bStudy population included pregnant women only

For 24 of the 26 studies, we extracted the variables included in the multivariable regression models used to obtain VE estimates (Additional file 2: Table S1); the remaining two studies did not clearly report these variables. All 24 studies with available information adjusted for age, and the majority adjusted for presence of high-risk conditions or comorbidities (n = 17; 71%) and calendar time (n = 15; 63%). Many studies also adjusted for time between illness onset and sample collection (n = 12; 50%), and sex (n = 10; 42%).

All of our included test-negative design studies were deemed to be at low risk of bias, and all included calendar time in their adjusted models [68, 15, 16, 1821, 2430, 32, 34, 36, 37]. The remaining case-control studies were also categorized as being at low risk of bias [17, 35], as were all the included cohort studies [22, 23, 31, 33]. Details of the evaluation of the included studies are provided in Additional file 3: Figure S1.

Among the 20 articles included in the meta-analysis, there were 16 analyses for influenza H1N1, 14 for H3N2, and 13 for B that compared VE among those vaccinated in both seasons to those vaccinated in the prior season only. When compared to vaccination in the prior season only, VE was higher for vaccination in both seasons for influenza H1N1 (∆VE = 25%; 95% CI 14%, 35%; I2 = 0%) and B (∆VE = 18%; 95% CI 3%, 33%; I2 = 26%), but not H3N2 (∆VE = 7%; 95% CI – 7%, 21%; I2 = 4%) (Table 2, Figs. 23, and 4). When stratified by influenza season, the results for all seasons were consistent with the overall results (Additional file 4: Table S2).

Table 2.

Comparison of vaccine effectiveness (VE) by vaccination group and influenza type/subtype

Vaccine effectiveness comparison Relevance of results H1N1 H3N2 B
Vaccinated both seasons versus vaccinated prior season only
ΔVEa (95% CI)
ΔVE = VEboth − VEprior only
Patient and policy perspectives 25% (14%, 35%) 7% (− 7%, 21%) 18% (3%, 33%)
Vaccinated current season only versus vaccinated neither season (reference group)
Pooled VEcurrent only
Patient and policy perspectives 62% (51%, 70%) 45% (35%, 53%) 64% (57%, 71%)
Vaccinated both seasons versus vaccinated current season only
ΔVEa (95% CI)
ΔVE = VEboth – VEcurrent only
Policy perspective 3% (− 8%, 13%) – 20% (− 36%, − 4%) – 11% (− 20%, − 2%)

Italic type-face indicates significant results

aΔVE > 0 implies higher vaccine effectiveness estimate when vaccinated in both seasons

Fig. 2.

Fig. 2

Comparison of VE estimates against influenza H1N1 in those vaccinated in both seasons versus those vaccinated in the prior season only

Fig. 3.

Fig. 3

Comparison of VE estimates against influenza H3N2 in those vaccinated in both seasons versus those vaccinated in the prior season only

Fig. 4.

Fig. 4

Comparison of VE estimates against influenza B in those vaccinated in both seasons versus those vaccinated in the prior season only

Sixteen analyses for influenza H1N1, 14 for H3N2, and 14 for B compared VE among those vaccinated in the current season only to those vaccinated in neither season. VE was higher for vaccination in the current season compared to neither season for influenza H1N1 (∆VE = 62%; 95% CI 51%, 70%; I2 = 26%), H3N2 (∆VE = 45%; 95% CI 35%, 53%; I2 = 0%), and B (∆VE = 64%; 95% CI 57%, 71%; I2 = 0%) (Table 2, Figs. 56, and 7). The results for individual seasons were consistent with the overall results (Additional file 4: Table S2).

Fig. 5.

Fig. 5

Comparison of VE estimates against influenza H1N1 in those vaccinated in the current season only versus those vaccinated in neither season

Fig. 6.

Fig. 6

Comparison of VE estimates against influenza H3N2 in those vaccinated in the current season only versus those vaccinated in neither season

Fig. 7.

Fig. 7

Comparison of VE estimates against influenza B in those vaccinated in the current season only versus those vaccinated in neither season

For the comparison of those vaccinated in both seasons to those vaccinated in the current season only, 16 analyses for influenza H1N1, 14 for H3N2, and 14 for B compared VE among from the 20 included articles. We observed no statistically significant VE difference between vaccination in both seasons and vaccination in the current season only for influenza H1N1 (∆VE = 3%; 95% CI – 8%, 13%; I2 = 0%). We observed statistically significant VE differences between vaccination in both seasons and vaccination in the current season only for influenza H3N2 (∆VE = − 20%; 95% CI – 36%, − 4%; I2 = 35%), and B (∆VE = − 11%; 95% CI – 20%, − 2%; I2 = 0%) (Table 2, Figs. 89, and 10). For the H3N2 comparison, the results for individual seasons were inconsistent with the overall result except for the 2014–2015 season (i.e., ∆VEs were not statistically significant in the comparison of both seasons versus current season for any season except for 2014–2015) (Additional file 4: Table S2).

Fig. 8.

Fig. 8

Comparison of VE estimates against influenza H1N1 in those vaccinated in both seasons versus those vaccinated in the current season only

Fig. 9.

Fig. 9

Comparison of VE estimates against influenza H3N2 in those vaccinated in both seasons versus those vaccinated in the current season only

Fig. 10.

Fig. 10

Comparison of VE estimates against influenza B in those vaccinated in both seasons versus those vaccinated in the current season only

To address overlapping patients in the 2010–2011 season analyses in Spain (one conducted in the Navarra region [20] and one that included eight regions in Spain [19]), we performed a sensitivity analysis removing the Navarra region study [20] from the H1N1 meta-analyses and found that it had no effect on the results for any of the three comparisons. When we removed the Navarra region study, we found that for H1N1 VEboth-VEprior only was 25% (95% CI 14%, 35%); VEcurrent only was 62% (95% CI 51%, 71%); and VEboth-VEcurrent only was 2% (95% CI− 9%, 13%). The original estimates for H1N1 were 25% (95% CI 14%, 35%), 62% (95% CI 51%, 70%), and 3% (95% CI− 8%, 13%), respectively.

Among the studies included in the qualitative synthesis but not the meta-analysis, two studies presented results using a definition of “prior season vaccination” that included multiple prior seasons and therefore did not meet the inclusion criteria for the meta-analysis [16, 26]. One of these studies considered vaccination history over two consecutive seasons using data from nine influenza seasons (2000–2001 to 2008–2009); those vaccinated in the current season only had the highest VE [26]. Finally, a study from the Navarra region in Spain that assessed vaccination over the current and two prior seasons showed a range of results [16]. Residual VE without current vaccination was noted if vaccinated in both the prior two seasons. For both influenza H3N2 and B, vaccination in the current season and one prior season resulted in quite low VE, whereas vaccination in the current and both prior seasons resulted in higher VE. VE against influenza B was highest among those vaccinated in the current season only compared to the other vaccination groups, whereas this group had the lowest VE against H3N2 [16].

Six studies [15, 16, 23, 26, 31, 32] presented results for any influenza rather than by influenza type/subtype, two of which were summarized above because they also used multiple prior seasons [16, 26]. There were five estimates from the four remaining studies not summarized above. Of these, three favored vaccination in the current season only, and two favored vaccination in both seasons. None of the estimates favored vaccination in the prior season only. In the one study that presented two VE estimates, seasonal differences were apparent. In the Southern Hemisphere 2011 season, the highest VE was observed among those who had been vaccinated in both current and prior seasons, but in the Southern Hemisphere 2010 season, the highest VE was observed among those who had received the current season vaccine only [32].

Discussion

We found that irrespective of a patient’s vaccination status for the prior season, current season vaccination is associated with greater protection against laboratory-confirmed infection by influenza H1N1 and B. This was evident comparing vaccination in both seasons to vaccination in the prior season only. Furthermore, compared to no vaccination for either season, individuals who received the current season’s vaccine had greater protection against all three influenza types/subtypes. Therefore, vaccination in the current season is generally the best option for the patient. Recent studies have raised questions about the impact of repeated vaccination [68], which is of concern to policy-makers with regard to annual influenza vaccination recommendations. Of relevance to the policy-maker (but not of pragmatic relevance to the patient, who cannot alter his/her vaccination history or predict future influenza strain circulation), we observed lower VE in those vaccinated in both seasons compared to only in the current season for influenza H3N2 and B, but not for H1N1. The 2014–2015 influenza season influenced the overall significance, where pooled VE across three studies was lower for those vaccinated in both the current and prior season compared to those vaccinated in the current season alone. However, this comparison does not account for increased susceptibility to influenza during the prior season due to being unvaccinated for that season. Based on the NOS, we assessed that the studies included in this review had a low risk of bias. However, the theoretical underpinnings of the test-negative design are still in the process of explication [3941], and there has not yet been a theoretical assessment of the potential biases in evaluation of repeated vaccine effects using the test-negative design.

The results of this review are not consistent with those found by Beyer and colleagues in 1999 [5]; their meta-analysis of seven field studies and 12 serologic studies found no significant difference between the single and multiple vaccination groups for all influenza subtypes combined. Our study differs from Beyer et al. by including studies that feature contemporary laboratory testing methods, influenza subtype-specific analysis, and study designs with consistent vaccination comparison groups. A recently published meta-analysis reported pooled VE estimates for the same vaccination status groups as our study (prior only, current only, both seasons) [42]. Similar to our study, that study found VE to be consistently lowest among those vaccinated during the prior season only. As well, for the 2014–2015 season, VE against H3N2 tended to be higher for those vaccinated in the current season only compared to those vaccinated during both seasons. However, that study did not examine the differences in VE as presented in this study.

In our review, the comparison groups used in the meta-analysis provided a more refined calculation of VE that accounted for recent vaccination history. Standard VE calculations (those that do not account for prior vaccination history of the vaccinated group) are comparing those vaccinated in the study season (a mixture of subjects vaccinated in the current season only and those with current and prior vaccination) to a reference group of those not vaccinated in the study season (which includes both those vaccinated in neither season and those vaccinated in the prior season only). Our study allowed for these vaccination groups to be analyzed separately to understand the impact of prior season’s vaccination on current season VE.

Our study was further strengthened by aligning the VE comparisons with patient and policy perspectives, in order to aid decision-making by patients, practitioners, and policy-makers. Additionally, by calculating the differences in VE between the various vaccination groups within each study, we controlled for any methodological biases unique to a particular study, such as study design or study settings (e.g., outpatient vs. hospital-based studies), since these biases would apply equally to each vaccination group. Thus, rather than first pooling the VE estimates from each vaccination group across studies and subsequently taking the difference, we pooled the differences obtained from VE estimates within each study. Finally, because VE can vary by age group and influenza type/subtype, this study was strengthened by the detailed stratification of results by type/subtype, as well as by using VE estimates for the most specific patient groups available (e.g., age-stratified groups rather than “all ages”).

This study also has some limitations. First, the analysis accounts only for vaccination status in one prior season. Results might differ when considering a patient’s vaccination history over a greater number of seasons, which is particularly important when considering the importance of influenza VE in older adults who potentially have received many years of consecutive vaccinations. McLean and colleagues found no difference when exploring VE over two consecutive seasons, but when they used a reference group with no vaccination over six seasons, those vaccinated in the current season only and not in the previous five seasons had the highest VE against influenza H3N2 and B, with progressively lower VE with increasing vaccines received over the previous five seasons [6]. Few studies reported on vaccination history beyond prior and current seasons, and they did not group history consistently, so further analysis incorporating the effects of serial vaccination from these studies was not possible, but is an important analysis to conduct in the future when more data are available. Second, our study did not account for past influenza infection, which may have provided some protective effect against laboratory-confirmed influenza in subsequent seasons [43]. A patient’s first exposure to influenza vaccination or infection can impact subsequent responses to vaccination or infection (referred to as original antigenic sin or back-boosting), which was not accounted for in this study [44]. Third, this study did not differentiate the types of influenza vaccines used for vaccination (e.g., live attenuated or inactivated; quadrivalent or trivalent; adjuvanted or unadjuvanted; high dose or standard dose). Given the differing types of immune response induced by these various products, different impacts of prior vaccination on current season VE may result. Fourth, we evaluated the absolute difference in VE, instead of looking at a ratio, which could be considered more appropriate given the scale on which VE is calculated. However, reporting ratios introduces other challenges, such as accommodating negative values and estimating confidence intervals. Since deriving practical conclusions for annual vaccine decision-making was the goal, we reported more intuitive differences in VE, as others have done previously [14, 45]. Finally, based on the limited available information in each study, we could not adjust for the match between the current season’s vaccine and the circulating strains, the prior season’s vaccine and the current season’s circulating strains, or changes in vaccine strains from one season to the other, all of which may affect VE from 1 year to the other as noted by Smith et al.’s antigenic distance hypothesis [46]. Skowronski et al. recently examined VE for influenza H3N2 in Canada using this framework and concluded the effects of repeated vaccination were consistent with the antigenic distance hypothesis [47]. We attempted to assess VE based on antigenic distance in the included articles by considering the vaccine strain and circulating strain match where possible, but not all studies provided detailed strain information. In the articles with sufficient information, the variation of vaccine and circulating strain matches were too few and were grouped by season, and as seasonal analysis was already included in our meta-analysis, no further information was gained. However, consistent with Skowronski et al.’s findings, we did find significant negative interference in the 2014–2015 influenza season, which supports the antigenic distance hypothesis which predicts that this would occur when vaccine strains are homologous from 1 year to the next but the prior season’s vaccine does not match the current circulating strain. Future VE studies should continue to incorporate vaccination status in prior seasons and provide as much detail as possible to allow assessment of the match between vaccine and circulating strains and the changes in vaccine strains over time. Future studies should also assess the impact of vaccination over multiple past seasons.

Conclusions

In conclusion, from the patient’s perspective, vaccination in the current season is generally the best option regardless of prior season vaccination. From a policy perspective, although VE was lower against H3N2 and B for individuals vaccinated in both seasons compared to those vaccinated in the current season only, this result may vary from season to season; in addition, it should be noted that past vaccination history cannot be altered and this comparison disregards susceptibility to influenza during the prior season among those vaccinated in the current season only.

Additional files

Additional file 1: (20.7KB, docx)

Database Search Strategy (DOCX 20 kb)

Additional file 2: (20.9KB, docx)

Table S1. Study characteristics of articles included in the meta-analysis and/or qualitative synthesis (DOCX 20 kb)

Additional file 3: (285.8KB, pdf)

Figure S1. Results of the risk of bias assessment by category using the Newcastle-Ottawa Scale (PDF 285 kb)

Additional file 4: (26.9KB, docx)

Table S2. Meta-analysis pooled results by influenza season and influenza type/subtype (DOCX 26 kb)

Acknowledgements

We acknowledge the Public Health Ontario scientific librarians for their assistance in developing the database search strategies and Dr. Lennon Li for his guidance in statistical analysis. Additionally, the authors would like to acknowledge the authors of all of the studies included in this review.

Funding

There was no funding source for this study.

Availability of data and materials

The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.

Abbreviations

CINAHL

Cumulative Index to Nursing and Allied Health Literature

NOS

Newcastle-Ottawa scale

PRISMA

Preferred Reporting Items for Systematic Reviews and Meta-Analysis

VE

Vaccine effectiveness

ΔVE

Absolute difference in vaccine effectiveness

Authors’ contributions

BFW had the idea for the review, and SAB and LCR managed the literature search and data extraction. BFW, JCK, RGS, SAB, and LCR developed the analysis plan. SAB and SF conducted the analysis and developed the figures. LCR wrote the original draft of the manuscript. BFW, JCK, SF, BJC, RGS, SAB, and LCR determined the study approach, interpreted the results, and critically reviewed the manuscript. All authors read and approved the final manuscript.

Ethics approval and consent to participate

Not applicable

Consent for publication

Not applicable

Competing interests

The authors declare that they have no competing interests.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Footnotes

Lauren C Ramsay and Sarah A Buchan are joint first authors.

Jeffrey C Kwong and Bryna F Warshawsky are joint senior authors.

Contributor Information

Lauren C. Ramsay, Email: lauren.ramsay@theta.utoronto.ca

Sarah A. Buchan, Email: sarah.buchan@mail.utoronto.ca

Robert G. Stirling, Email: rob.stirling@canada.ca

Benjamin J. Cowling, Email: bcowling@hku.hk

Shuo Feng, Email: shuofeng@connect.hku.hk.

Jeffrey C. Kwong, Email: jeff.kwong@utoronto.ca

Bryna F. Warshawsky, Email: bryna.warshawsky@oahpp.ca

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

Additional file 1: (20.7KB, docx)

Database Search Strategy (DOCX 20 kb)

Additional file 2: (20.9KB, docx)

Table S1. Study characteristics of articles included in the meta-analysis and/or qualitative synthesis (DOCX 20 kb)

Additional file 3: (285.8KB, pdf)

Figure S1. Results of the risk of bias assessment by category using the Newcastle-Ottawa Scale (PDF 285 kb)

Additional file 4: (26.9KB, docx)

Table S2. Meta-analysis pooled results by influenza season and influenza type/subtype (DOCX 26 kb)

Data Availability Statement

The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.


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