Paediatric rotavirus vaccination, coeliac disease and type 1 diabetes in children: a population-based cohort study

We applied a cohort design to prospectively collected healthcare data from the Clinical Practice Research Datalink (CPRD) Aurum. CPRD Aurum contains data relating to health and healthcare utilisation from people registered at a network of general practices across the UK. This is a de-identified register of approximately 13 million current patients across the UK [18]. Patients registered in CPRD Aurum are representative of the population with regard to demographic factors, geographical distribution and level of deprivation [19]. Individual-level de-identified data were extracted from CPRD Aurum in May 2020.

In this study, we included children registered with CPRD Aurum who were born in the UK between 01 January 2010 and 31 December 2015 and registered at a CPRD GP practice within 14 weeks of birth. Additionally, we only included participant records which met CPRD Aurum quality standards regarding valid age, sex and registration period. In order to account for vaccine hesitancy as a potentially confounding factor, we only included children in the study with a record of DTaP/IPV vaccination [20, 21]. We used this as a proxy measure of vaccine hesitancy because this vaccine has been a long-standing part of the routine childhood immunisation schedule in the UK. All participants who met these criteria were included in the cohort.

Participants entered the follow-up period at 6 months of age (UK vaccination schedule upper limit for second dose of Rotarix®). Participants exited the cohort if they were recorded as having the outcome, or on their seventh birthday if they did not have the outcome. If the participants transferred out from the GP practice, died, were recorded as experiencing rotavirus gastroenteritis or had a last recorded data collection date before their seventh birthday, they exited the cohort.

In this study, the primary outcomes were CD and T1D. CD was defined based on either a recorded diagnosis of CD or the prescription of gluten-free goods [22]. T1D was defined based on a recorded diagnosis of T1D [23]. The primary exposure was rotavirus vaccination, a binary variable defined as having a record of one or more doses of Rotarix® in CPRD Aurum records. The list of CPRD Aurum codes used to classify the primary exposure variable, the two outcome variables and DTaP/IPV vaccination status for study inclusion have been published as an open-source document [24].

One of the key potential biases in this study was the increased awareness and diagnostic testing for both outcomes over this time period. In order to adjust for this, we included a year of birth variable in our analysis and also conducted sensitivity analyses including only those born post vaccine introduction in 2013.

Another potential bias affecting observational studies assessing vaccines with high uptake is the bias related to healthcare access. This bias has previously been demonstrated in a study assessing rotavirus vaccine effectiveness in the UK [20]. Given that both outcomes are chronic conditions rather than an acute illnesses, they may not have been present in the same way. We assessed the potential presence of this bias by estimating the association between the rate of GP consultations and both primary outcomes (CD and T1D).

We estimated sample sizes in Stata 15 (StataCorp LLC: College Station, TX), using the exponential test comparing two independent hazard rates. We specified a follow-up period of 6 years, with loss to follow-up of 0.5 over 3 years, α of 0.05, using 80% power and a 1:1 ratio of comparison groups.

Prevalence of CD in children under the age of seven is estimated to be 1% [25, 26]. However, only a quarter of cases are likely to be diagnosed and a recent study estimated CD prevalence to be 0.15% [27]. For T1D in children under the age of seven in the UK, we assumed a prevalence of 0.1% [4]. Therefore, we conducted sample size calculations assuming 0.15% prevalence for CD and 0.1% for TD1. In order to observe a 20% reduction in hazard, we calculated this would require 435,470 participants for CD and 652,988 participants for T1D.

The primary outcomes in this analysis were CD and T1D, both binary outcomes for each participant. We used a survival analysis to account for differential person-time at-risk and used hazard ratios (HR) as our measure of association. We used a Kaplan-Meier estimator to visualise the survival function of exposed and unexposed groups. Time at risk was defined as days since the participant entered the cohort at six months of age. We used a mixed-effects Cox regression model to estimate the relationships between the hazards of CD, T1D and a range of explanatory variables. Random GP practice-level intercepts were included to accommodate unmeasured differences in explanatory variable and outcome recording between practices. To build the multivariable model, we initially included all explanatory variables identified as scientifically relevant, then added other explanatory variables, retaining them in the model if they improved model parsimony, as measured using the Akaike Information Criterion (AIC). We tested the proportional hazards assumption of the semi-parametric Cox model and checked for interactions between explanatory variables.

In addition, we conducted a sensitivity analysis which included only those born post vaccine introduction in July 2013 in order to analyse to the effect of increased awareness and diagnostic testing in this later follow-up period. We also conducted another sensitivity analysis which did not right-censor person-time at-risk at participants’ seventh birthdays, to examine any potential impact on older children. We conducted all analyses using R version 3.6.1 (R Core Team: Vienna, Austria), using the survival and coxme packages [28, 29].

The study dataset extracted from CPRD Aurum contained 926,013 participants. After applying study inclusion criteria, the cohort contained 880,629 participants. Of these, 429,673 (48.8%) were female and the most common geographical locations were London (20.6%) and West Midlands (16.7%). Participants were registered at a total of 890 GP practices. A total of 343,113 (39.0%) participants had rotavirus vaccination; in those born after the introduction of routine rotavirus vaccination, 93.4% were vaccinated. Of those with rotavirus vaccination, 19,413 (5.7%) received only one dose. We also found that participants were recorded having 1317 episodes of rotavirus gastroenteritis. For a full description of cohort characteristics and explanatory variable distributions, please see Table 1.

When we explored the relationship between rotavirus vaccination and other explanatory variables, all of these variables, apart from sex (p = 0.719), were associated with vaccine status. Due to the introduction of the rotavirus vaccine into the routine immunisation schedule in 2013, there was an association with year of birth (p < 0.001). Children with rotavirus vaccination also had a higher mean rate of GP consultations per year (7.63) than children without rotavirus vaccination (7.08, p < 0.001). There was an association between rotavirus vaccination and geographical location (p < 0.001) and rotavirus vaccination and IMD quintile of residence (p < 0.001).

Study participants contributed a total of 4,388,355 person-years at-risk, with the median follow-up period being 5.66 person-years per participant. The cohort follow-up period started on 26 March 2010 and ended on 28 April 2020. The outcome of CD was recorded for 1657 participants, an incidence rate of 38.0 cases per 100,000 person-years at-risk. The median age at diagnosis of CD was 3.2 years for participants in this cohort. T1D was recorded for 733 participants, an incidence rate of 17.1 cases per 100,000 person-years at-risk. The median age at diagnosis of T1D was 3.3 years for participants in this cohort. The two outcomes were not mutually exclusive; CD was also diagnosed in 54 of the 733 participants with T1D (7.4%)

The Kaplan-Meier survival estimators for CD and T1D, stratified by rotavirus vaccination status, are shown in Fig. 1. For both CD and T1D, due to the large proportion without the outcome, calculation of median survival time was not relevant. Based on visual inspection of both Kaplan-Meier plots, the hazards in both groups were proportional.

The results of mixed-effects Cox regression modelling, with random intercepts for GP practices, are shown in Table 2. In univariable analysis the HR for the association between rotavirus vaccination and CD was 0.93 (95% CI 0.84–1.04), when simultaneously adjusted for other explanatory variables, the HR increased to 1.05 (95% CI 0.86–1.28). Sex was associated with CD in both univariable and adjusted models, with females having 40% higher hazard than males (p < 0.001). Rotavirus vaccination was not associated with T1D in either univariable analysis (HR 1.01, 95% CI 0.87–1.19), or when adjusted for confounders in multivariable analysis (HR 0.89, 95% CI 0.68–1.19).

Sensitivity analysis results are shown in Table 3. Restricting the cohort to only those born after 1st July 2013 had a minor effect on the point estimates. Removing censoring of follow-up time at the seventh birthday did not change the association between rotavirus vaccination and CD or the association between rotavirus vaccination and T1D.

One of the key strengths of this study is that it uses CPRD Aurum data. Patients at GP practices enrolled in CPRD are representative of the population in England with regard to age, gender, geographical spread and deprivation [19]. Because this sampling frame of CRPD Aurum patients is representative of the population of England, it would be reasonable to infer that the study findings are generalisable to the wider population. The size of the CPRD Aurum database meant that it was feasible to include over 880,000 participants in this study, exceeding the calculated sample size.

Another strength of using CPRD Aurum data is the completeness and detail of information it contains. CPRD Aurum routinely undertake data validation and quality assurance work on their database [19]. This meant that we were able to exclude potential participants where their data did not meet CPRD Aurum quality standards, improving confidence in the completeness and reliability of this data source.

Regarding the use of CPRD Aurum records as a measure of CD and T1D diagnoses, a similar approach of using diagnostic codes for CD in CPRD Aurum data was used previously [2]. It is possible that this approach underestimates CD and T1D incidence by missing cases diagnosed in secondary care and entered in GP notes as free text. However as participant-level free-text records were not available from CPRD Aurum due to privacy concerns, this meant that it was not possible to formally validate this method for our diagnoses.

One trend which was relevant for this analysis is the increase in the incidence of CD diagnoses over time in England; CD increased from 5.16 cases per 100,000 in 1990 to 19.14 cases per 100,000 in 2011 [2]. Although these data do not cover most of the follow-up period in this study, from 2010 to 2020, it may be inferred that these trends have continued. Compared to CD, T1D incidence in children in England has remained stable since 2013 [4]. The increase in the rate of CD diagnoses may have affected the reliability of using CPRD Aurum as the recording as the recording of these diseases may have changed over time. This may have created a potentially confounding relationship as time was also associated with the probability of being vaccinated against rotavirus. One of the strengths of this analysis was that we attempted to adjust for this by including year of birth as an explanatory variable; however it is possible that some residual confounding remained.

Another strength of the study was the inclusion of socio-economic deprivation data. This was an important confounder as rotavirus vaccination coverage in the UK has been shown to be lower in more deprived socio-economic groups [14], and CD incidence has been found to be lower in the most deprived people [2]. This was consistent with our finding that the risk of CD was lower in those in IMD quintiles 4 and 5 (the most deprived).

A key limitation of this study relates to the period of follow-up in which we measured the diagnosis of CD and T1D. In this study, we used a 7-year follow-up period; this was the maximum period for those born since the introduction of routine rotavirus vaccination in July 2013. This was relevant because the incidence of CD and T1D changes with age. CD is relatively higher in those under five, then decreases and increases again in those aged over 30 [2]. T1D incidence is low in those under 2 years of age, then increases between the ages of two and ten [38]. We used a sensitivity analysis to examine the impact of removing right-censoring at 7 years; however, as very few children born before July 2013 were exposed to rotavirus vaccine, this follow-up period of 7 years limits the inference which could be made from this study on the association between rotavirus vaccination and both CD and T1D diagnosed later in life. The impact of this 7-year follow-up period on the size and direction of results is uncertain. Should cases of CD and T1D continue to occur at similar proportions in older ages, these results would continue to apply. It could however be the case that a biological mechanism for rotavirus vaccination to protect against CD and/or T1D manifests later in life, and is not captured by this study. Subsequent follow-up of this cohort over a longer time period would be an effective method for addressing this issue.

In this study we analysed exposure as a binary variable; with exposure being based on having one or more rotavirus vaccinations. This is consistent with previous rotavirus research in England [14]; however, there are two doses recommended in the routine schedule, so it could be viewed as a limitation that we did not analyse the two “levels” of vaccination separately. Finding a dose-response relationship would have been valuable in providing evidence that a potential association is causal. However, in this study it was not possible to analyse this as the number of participants only receiving one dose was so small (5.7%).