Clinical and Economic Burden of Pediatric Mild-to-Moderate Atopic Dermatitis: A Population-Based Nested Case–Control Study in Sweden

Two population-based Swedish registries, the National Patient Register (NPR), and the Prescribed Drug Register (PDR) were used in this study. Both registers are governed by the Swedish National Board of Health and Welfare and use a common and unique identification number for each individual, enabling patient-level linkage between registries. The data used in this study were anonymized. This implied that the granularity of certain variables was limited to ensure the anonymity of the patient. Specifically, this meant that the date of secondary care visits and dispensation was provided on a yearly level, age was available in age groups of five (0–4, 5–9, etc.) and Anatomical Therapeutic Chemical (ATC) codes were truncated to a three-digit level.

The NPR contains information on all secondary care (care visits, either outpatient visit or inpatient hospitalization with referral from primary care) in Sweden and data for year of visit, gender, age, and main diagnosis (atopic dermatitis or other diagnosis) were collected for each study participant between 1 January 2001 and 31 December 2017. The PDR contains information on all drug dispensations (originating from both primary and secondary care) filled at pharmacies in Sweden. Data for the ATC code (truncated to three digits), the year of dispensation, and cost of the dispensation for each study participant between 1 July 2005 and 31 December 2017 was collected from the PDR. The cost of dispensed drugs was extracted directly from the PDR which contains the publicly available list prices. All types of dispensed drugs were included in the calculation of total direct medical costs. Cost of drugs was inflated to the 2018 price level using the Swedish consumer price index and then converted into euros using the average exchange rate of SEK/€ during 2018 (€1 = 10.31 SEK). Unit costs of secondary care visits (differentiated between AD visit and non-AD visit) were extracted from several Swedish regional price lists [22‐28] to ensure accurate prices which may vary across regions.

This study was approved by the Regional Ethical Review Board in Gothenburg (Dnr: 2019-02986) and performed in accordance with the ethical standards in the 1964 Declaration of Helsinki and its later amendments. For this type of study, individual formal consent was not required.

This was a retrospective, observational nested case–control study including children aged 0–14 (inclusive) in Sweden with either a primary diagnosis of AD (ICD-10 code L20+ or L30.8C) in secondary care, or by dispensation of two (within 12 months of each other) topical corticosteroids (TCS), or a topical calcineurin inhibitor (TCI) between 1 January 2009 and 31 December 2017. A schematic outline of the study design is provided in Fig. 1. Patients identified through a dispensation (TCS or TCI) were identified from the PDR which contains all dispensations for primary and secondary care. Hence, patients could be included either through diagnosis code (using the International Classification of Diseases, ICD-10) in secondary care and/or a drug dispensation originating from secondary or primary care. Treatment with TCS drugs is indicated for several skin conditions (including other types of dermatitis and psoriasis), and TCS dispensation alone is a poor predictor of AD diagnosis [29]. Therefore, subjects with hospital visits related to other types of dermatitis or medical conditions known to lead to the use of TCS were excluded from the study population. Diagnosis codes which required exclusion are listed in Table S.I in the supplementary material. In addition to excluding patient-based diagnosis codes to further refine the study population, patients with dispensations of TCSs used in other types of dermatitis or to treat vaginal fungal infection, antipsoriatics or salicylates for dermatological use were also excluded from the study population. ATC codes which required exclusion are listed in Table S.II. The exclusion algorithm used in this study was based on a previously published study in Sweden [5]. This study used the European classification system for the potency of corticosteroids which includes four levels (I–IV) in ascending order of potency [30].

As severity of the disease is not coded in administrative registers, this study defined severity based on concurrent treatment employed in a previously published study [31]. Patients with systemic treatments (corticosteroids and non-corticosteroid immunosuppressants) were considered to have a severe form of AD and are presented separately in this publication for reference [31].

The pM2M AD cohort was matched by age and gender to a random sample (reference cohort) from the Total Population Register held by Statistics Sweden. The register covers the entire Swedish population from 1968 and contains basic demographic and socioeconomic information on the individual level. In this study, the register was only used to identify the reference cohort and no information was extracted. The two cohorts (the pM2M AD and reference cohort) were mutually exclusive and had equal lengths of follow-up.

The date of inclusion was selected as the patient’s index date and is a proxy for the start of clinically diagnosed AD or a new episode with AD-care visits and/or treatment (after a look-back period of at least 3.5 years without treatment in primary or secondary care and/or a secondary care visit due to AD). Patients were followed from index date until the end of study period on 31 December 2017. Date of death was not available in this study and thus not controlled for. Each reference individual was allocated the same index date as their matched case. This implied that each case and corresponding reference had identical follow-up. Demographic characteristics and treatment type (case cohort) were described at the index date.

Healthcare resource use was observed annually from index date until the end of the study period. All secondary care visits (AD- and non-AD-related) were included, and the incidence rate ratio (IRR) of secondary care visits between the pM2M AD cohort and reference cohort was calculated annually by dividing the number of secondary care visits per year in the pM2M AD cohort by the number in the reference cohort. Total direct medical costs, including cost of all AD-related and non-AD-related secondary care visits and dispensed drugs were calculated annually in all cohorts. The cost of secondary care visits was calculated by multiplying each secondary care visit by one of the following costs: €275 per AD-related outpatient visit, €279 per non-AD-related outpatient visit, €546 per day of AD-related inpatient hospitalization, and €661 per day of non-AD-related inpatient hospitalization. A visit was considered AD-related if the primary diagnosis was either L20+ or L30.8C. Cost of dispensed drugs was extracted directly from the PDR.

The number (n), mean, and standard deviation (SD) were presented for continuous variables while the number and percentage were presented for categorical variables. Comparisons between the pM2M AD and the reference cohort were evaluated using statistical tests with an a priori significance level of alpha = 0.05. An independent two-group t test was used to compare means for continuous variables, and a chi-square test to compare proportions for categorical variables [32]. Statistical comparisons were made within years between patients and reference individuals, but comparisons across years were not performed. All analyses were performed in Stata (StataCorp. 2019. Release 16. College Station, TX, USA: StataCorp LLC.).

A total of 99,300 patients were included in the two case cohorts through a secondary care diagnosis of AD, a TCS dispensation, and/or a TCI dispensation according to previously used criteria [5]. Of these, 11.7% (11,609) received systemic treatments during the study period and were deemed to have severe AD. The remaining 87,721 patients were considered to have mild-to-moderate AD. An equal number (87,721) of reference individuals were included in the reference cohort.

Baseline characteristics for the mild-to-moderate cohort, the severe AD cohort, and the reference cohort at index date are presented in Table 1. At index date, 67.5% of pM2M were between 0 and 4 years old, and 53.2% were male. In the severe subgroup, patients were older, and 57.6% were male. A majority of AD patients were identified through a TCS dispensation, 89.1% and 89.7% in the pM2M and severe AD cohort, respectively.

The pM2M AD cohort had a larger number of secondary care visits (for any reason) on average than the reference cohort during all years of follow-up. In the index year, the average number (SD) of all secondary care visits was 2.25 (3.36) and 0.96 (2.14) per patient in the pM2M AD and reference cohort, respectively (Fig. 2). Most secondary care visits were outpatient visits (94.5%), while hospitalizations were uncommon (5.5%). The severe AD cohort had on average 3.14 (6.16) secondary care visits in the index year. The largest IRR between the pM2M AD cohort and the reference cohort was found in the first two years (2.35 and 1.91, respectively) following index and ranged between 1.56 and 2.35 (P < 0.001) for up to 1–5 years after disease onset. Similarly, the average number of drug dispensations (any drug) was also larger in the pM2M AD cohort compared with the reference cohort throughout the follow-up. During the index year, the pM2M AD cohort received on average 12.50 pharmacy dispensations per patient while reference individuals on average received 3.39 pharmacy dispensations per patient (data not shown). Patients in the severe AD cohort received on average 17.90 dispensations in the index year. The mean difference in healthcare resource use (both in terms of secondary care visits and dispensed drugs) between the pM2M AD and the reference cohort was statistically significant (P < 0.001) in all years. Detailed statistics are reported in Table S.III in the supplementary material section.

Given the larger healthcare resource use in the pM2M AD cohort, direct medical costs were consequently also larger in the pM2M AD cohort compared with the reference cohort. During the index year, the average direct medical costs were €587 higher per patient in the pM2M AD cohort compared with that for patients in the reference cohort. The average direct medical cost (SD) in the pM2M AD cohort was €1111 (3416), and €524 (2446) in the reference cohort. The corresponding estimate in the severe AD cohort was €1906 (7067). The cost of secondary care visits for patients in the pM2M AD cohort (€428 per patient) represented 73% of the incremental direct medical costs, while the cost of dispensed drugs (€159 per patient) represented the remaining 27%. Five years following index date, the cumulative difference in total direct medical costs was €118.9 million (€1663 per patient) for the entire pM2M cohort. Detailed statistics are reported in Table S.IV in the supplementary material section.

The cost burden of pM2M AD patients reported across other studies varies substantially (between €49 and €1519), likely due to differences in study design (retrospective, prospective, and survey), study setting (inclusion of reference cohort), and type of cost (drugs, primary and secondary care visits, out-of-pocket expenses, indirect costs). These differences make comparisons between studies difficult. The estimated cost burden of pM2M AD in the present study appears to be within the range of cost burden reported in the published literature. A German study that included children used a similar study design as the present study (retrospective with 8-year follow-up), and reported an  average annual cost for AD of €194 in mild patients and €417 in moderate patients [20]. The average annual cost per patient (over 5 years) in the present study was €224. Another retrospective study in a French setting reported the average cost of medications per patient used during the first year of follow-up to be €175 in the eczema cohort compared with €99 in the reference individuals. The average cost of dispensed drugs in this study was €225 and €67 per patient in the pM2M AD cohort and reference cohort, respectively [35]. Two Nordic studies (survey and prospective study) included cost of primary and secondary care visits together with cost of medications [36] and indirect cost [37], but neither differentiated results by severity. The survey study estimated the incremental cost of patients experiencing eczema symptoms at €410, while the prospective study estimated the incremental cost at €291. Finally, an Italian survey reported an annual average cost of €900 in mild patients and €1519 in moderate patients [19].

A major strength of this study is the use of two large national databases with complete population-level coverage to identify the study population. This study, therefore, provides a complete account of healthcare resource use in secondary care and for dispensed drugs originating from both primary and secondary care.

Three key factors contribute to possible bias in the study results. First, initial contact with the healthcare services in Sweden for mild, non-acute diseases is often in primary care. The present study collected primary care data for dispensed medications but not for diagnoses. Therefore, the complete economic burden of mild-to-moderate AD is likely higher than estimated in this study since this study does not include the cost of primary care visits and most patients with mild-to-moderate atopic dermatitis are treated by primary care physicians.

Second, the date for first dispensation of a TCS/TCI or a diagnosis in secondary care was used as the index date rather than the date of primary care diagnosis. This means that patients treated solely with emollients or lowest-potency TCS medications were not included in this study since these agents are available as over-the-counter drugs in Sweden and hence not captured by the PDR. From this perspective, the results in this study may therefore overestimate the economic burden since these “mildest” mild-to-moderate patients are likely to incur less than average healthcare resource use compared with the average mild-to-moderate AD patient. On the other hand, emollients are the basis of treatment for AD in all severities and the cost of these is not captured by this study.

Third, severity based on clinical assessment was not available in the administrative registers used in this study. Therefore, the definition of mild-moderate and severe AD was based on treatment class (topical, systemic, phototherapy) where information on potency and treatment concentrations was not available. This may have led to misclassification as we could not distinguish drugs with respect to potency within the class of TCS or concentrations within the class of TCIs since we only had access to the first three digits of the ATC codes in the database. Additionally, misclassification may have occured as mild-to-moderate patients with a flare may have been treated temporarily with systemic treatments or may have received phototherapy (this was not available in the database), or severe patients may not have received systemic treatment for unknown reasons. Although it was not possible to validate the severity classification, it follows treatment guidelines and the percentage of severe patients in this study (11.7%) is in line with other studies [2].

In addition, date of death was not included in this study, and therefore patients were not censored at death. Since the study population consisted of pediatric patients, this likely had a minor impact on the study results. In addition, this study only accounted for direct health care costs and did not include other types of costs, such as indirect costs associated with loss of school days. Finally, another limitation in this study was the inability to verify the sensitivity and specificity of the inclusion and exclusion criteria employed to identify AD cases from prescription data. However, the algorithm used in this study was developed by specialists in dermatology, pharmacoepidemiology, and biostatistics and has been validated in a Danish setting, yielding a sensitivity and specificity of 74.1% and 73.0%, respectively [38].