Health- related quality of life and self-worth in 10-year old children with congenital hypothyroidism diagnosed by neonatal screening

The Dutch neonatal CH screening method is primarily based on the measurement of T4 in filter paper blood spots. In 1992 and 1993 sampling was performed between 5 and 8 days after birth. T4, expressed as standard deviation score, is compared to the day mean. If T4 was ≤ −0.8 SD, thyrotropin (TSH) was additionally measured. When T4 was ≤ −3.0 SD or TSH was ≥50 μU/ml children were referred immediately. Children with a dubious result (−3.0 < T4 ≤ −2.1 SD, or 25 ≤ TSH < 50 μU/ml) underwent a second heelpuncture and were referred if the result was again dubious, or abnormal. The etiological classification of CH was based upon initial presentation, thyroid function determinants and thyroid imaging.

In 1992–93 Dutch pediatricians were advised to start with T4-supplementation in a dose of 6 to 8 μg/kg.day. In accordance with international guidelines T4-dose adjustments were based on thyroid function determinants, obtained at regular outpatient follow-up visits.

The complete cohort of patients with CH born in The Netherlands in 1992 and 1993 consisted of 141 patients (Table 1). Patients were classified as CH-T (CH of thyroidal origin), CH of central origin (CH-C) or CH not yet specified. CH-T was further classified as CH-T due to thyroid agenesis, thyroid dysgenesis, or thyroid dyshormogenesis. In this study, only children with CH-T were included.

From the original cohort 3 patients had died, 4 had moved abroad and 4 had transient CH. The parents of the remaining 130 patients were contacted via their pediatricians, whose responses led to the exclusion of patients with CH-C (n = 15), with a known or suspected syndrome (n = 9), with a brain tumour (n = 1), and patients of whom the mother was treated with T4 during pregnancy (n = 2). Three patients were excluded because the recommended dose adjustments were not made in time due to misunderstandings (Table 1, ‘not suitable’ to participate). Furthermore, the parents of 18 patients declined participation (Table 1, ‘not willing’ to participate). Parents of a total of 82 patients gave their written informed consent. To ascertain that the participating patients were well-treated (i.e. TSH 0.4-4.0 μU/ml) at the time of testing, the most recent measurement of thyroid function prior to the psychological tests was evaluated and if necessary T4-dose was adjusted. This resulted in dose adjustments for 20 patients. Patients were classified to subgroups based on their pre-treatment FT4 concentration: ‘severe CH’: FT4 ≤ 0.3 ng/dL (≤4 pmol/L), ‘moderate/mild CH’: FT4 > 0.3 ng/dL (FT4 > 4.0 pmol/L). The reference range for FT4 is 0.9-2.2 ng/dL (12–28 pmol/L) for children aged 2–6 weeks.

All children and their parents were asked to complete the questionnaires in the Academic Medical Center (AMC) (except for 7 patients who were tested in their local hospitals) under the supervision of the same psychologist (LvdSV), who was blinded for the patients’ medical details. The assistance of the psychologist was restricted to explaining the meaning of difficult words. The study protocol was approved by the institutional review board of the Emma Children’s Hospital/Academic Medical Center and the privacy committee of the Dutch CH Screening Board.

Data were analysed using SPSS version 12.0 (SPSS Inc., Chicago, IL). Before conducting the final analyses several preparation analyses were conducted. Firstly, scale scores were computed and missing data imputed on the basis of the guidelines of the TACQoL [17]. In calculation of the scale scores, one missing combined-item score was allowed for. The missing score was replaced by the mean value of the non-missing item scores. Second, the internal consistencies (Cronbach’s alphas) of the scales were calculated, and the distributions of the scale scores were considered.

HRQoL and self-worth of the group with CH were compared with that of the norm population in two ways: (1) using mean scale scores, (2) using the percentage of children at risk of impaired HRQoL and self-worth. Patients with CH (total group) were compared to the norm population, and thereafter the severe and moderate/mild subgroups as well. Differences between the severe and moderate/mild subgroups with CH were also tested. Analyses of covariance (ANCOVA) were conducted to test for differences on the TACQoL mean scale-scores between the group with CH and norm population and between the severity groups, corrected for gender. Because the database of the CBSK norm data was not available, we used the mean scores that were presented in the manual of the CBSK. Therefore one sample t-tests were performed to test whether the several CBSK-scales scores (means) of the children with CH differed from the means in the norm population [24]. Patients with CH (total group) were compared to the norm population, and thereafter the severe and moderate/mild subgroups as well. Differences between the severity groups regarding the CBSK-scale scores were tested with ANCOVA. To adjust for multiple testing, we used a Bonferroni correction and adjusted the alpha to 0.007 (0.05/7) for the TACQoL and 0.008 (0.05/6) for the CBSK. Effect sizes (d) were calculated by dividing the difference in mean score between the patients with CH (total group) and norm population by the standard deviation of the scores in the norm population. We considered effect sizes up to 0.2, 0.5, and 0.8 to be small, moderate and large respectively [28].

To create a clinically meaningful distinction, children with CH are categorized into being ‘at risk’ or ‘not at risk’ for problems (i.e. impaired HRQoL, impaired self-worth), based on percentile norms by age and gender in the norm population. The value of the 25 ^th percentile in the norm population was used for the scales of the TACQoL. Although there is no gold standard for good or bad HRQoL yet, this definition is considered to be a suitable way to differentiate between individuals with higher scale scores from individuals with lower scale scores [29]. The percentage at risk in the group with CH was compared with the percentage in the norm population using Chi-square tests (χ²-tests, p < 0.007;0.05/7). The definition of being at risk for impaired self-worth was based on the value of the 15 ^th percentile (CBSK scales) in the norm population as recommended in the manual of the CBSK [24]. We tested whether the percentage of children with CH with scores below the value of the 15^th percentile in the norm population was different from 15% using binomial tests (p < 0.008; 0.05/6).

Linear regression analyses were conducted to explore the influence of disease factors (initial FT4 plasma, age at onset therapy, initial T4 dose) on HRQoL and self-worth. Regression models were also fitted for HRQoL and self-worth predicted by full scale IQ, and predicted by motor skills (total score). All regression models were corrected for gender. A significance level of 0.007 (0.05/7) was used for the HRQoL scales and 0.008 (0.05/6) for the scales of self-worth. Because of the explorative nature of the regression analyses, regression coefficients at p < 0.05 and p < 0.01 were also reported, to be considered as a trend.

The characteristics of the participating patients with CH and their parents are given in Table 2. Of the 82 patients with CH (53 girls, 65%), 41 had severe CH and 41 had moderate/mild CH. The median age at start of T4 supplementation was 20 days for the total group. The IQ scores of the participating patients with CH are given in Table 2. For all details, we refer to a previous publication [3].

With respect to the self-worth only one significant difference was found (Table 4). The girls with CH reported lower social acceptance than the girls in the norm population; T = (1,50) = −2.75, effect sizes (d) = 0.4.

There were no significant differences found between the severity groups for HRQoL and self-worth (Table 3 and 4).

Patients with CH (total, severe, moderate/mild) showed higher percentages at risk for impaired self-worth than the norm population with regard to school competence and athletic competence; ranging from 27 to 34% versus 15% in the norm group (Table 6).

The regression analyses demonstrated only one significant result: higher full scale IQ was found to be correlated with better (parent reported) cognitive functioning (β = 0.38; p = 0.001).

Several trends could be reported, based on significance levels of 0.01 and 0.05. Regarding the disease factors, higher initial T4 dose was associated with better (parent-reported) physical HRQoL (β = 0.37; p < 0.05). Furthermore, higher full scale IQ was found to be correlated with better HRQoL regarding (child reported) negative emotions (β = 0.28; p < 0.05) and (parent reported) positive emotions (β = 0.23; p < 0.05). Finally, better motor skills were associated with higher (parent reported) HRQoL scores on motor functioning (β = 0.24; p < 0.05) and autonomy (β = 0.30; p < 0.01), and with better self-worth; social acceptance (β = 0.24; p < 0.05) and athletic competence (β = 0.29; p < 0.05).

This study has shown that children with CH, diagnosed by neonatal screening, are at increased risk for impaired quality of life and self worth. In particular, our findings add to the evidence for motor and cognitive problems in relation to CH. Following this, we can conclude that children with CH are vulnerable and that there is need for specific care. We believe that these results deserve proper attention and awareness of physicians treating these children. Furthermore, patients with CH and their parents should become more aware of the possible negative consequences of growing up with CH. Follow-up of patients with CH should not only be a medical/biochemical evaluation but, also to attain the best achievable quality of life. The focus during the follow-up should shift to attention to school performances, social-emotional functioning and supporting the patients. Therefore routine monitoring HRQoL and social-emotional functioning in children with CH is recommended. Incorporating patient reported outcomes of HRQoL in daily clinical practice will contribute to better communication with health care professionals and makes it easier for them to refer to the needed care if necessary [39, 40]. In addition, the use of valid and reliable screening instruments to detect patients with CH at risk for social, emotional and behavior problems are recommended, for example the Strength and Difficulties Questionnaire (SDQ) [41]. When motor problems are present, patients should be motivated to engage in sport activities or should be referred to the physiotherapist if needed. When cognitive problems are present, psychological examination would be useful and if necessary, intervention programs that improve cognitive functions such as memory and attention functioning or speech training might thereafter be offered to particular individuals. Finally, it seems important to stimulate children’s social performance and to support children with their social skills.