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Ann Pediatr Endocrinol Metab > Volume 26(4); 2021 > Article
Rho, Kum, Seo, Shim, Lee, and Hwang: Long-term outcomes of Graves’ disease in children and adolescents receiving antithyroid drugs

Abstract

Purpose

Antithyroid drugs (ATDs) are primarily used as an initial treatment in pediatric patients with Graves’ disease (GD). We aimed to investigate the long-term outcomes in pediatric GD patients receiving ATDs.

Methods

Retrospective data from a single center were collected from April 2003 to July 2020. A total of 98 children and adolescents aged 2–16 years diagnosed with GD and receiving ATDs was enrolled. We investigated the factors correlated with remission by comparing children who achieved remission after 5 years and those with persistent disease.

Results

The study included 76 girls (77.6%) and 22 boys (22.4%). During the 5-year follow-up period, 18 children (18.3%) maintained remission, ATDs could not be discontinued in 74 patients (75.5%), and relapse occurred in 6 patients (6.2%). The remission group had significantly lower thyroid-stimulating hormone-binding inhibitory immunoglobulin (TBII) level at diagnosis (P=0.002) and 3 months (P=0.002), 1 year (P=0.002), 2 years (P≤0.001), 3 years (P≤0.001), 4 years (P≤0.001), and 5 years (P≤0.001) after ATD treatment than did the nonremission group. The remission group also had a shorter time for TBII normalization after ATD treatment (P≤0.001). Multiple logistic regression analysis showed that the time to TBII normalization (cutoff time=2.35 years) was related to GD remission (odds ratio, 0.596; 95% confidence interval, 0.374–0.951).

Conclusions

TBII level and time to TBII normalization after ATD treatment can be used to predict remission in pediatric GD patients.

Highlights

TBII level at diagnosis, and during ATD treatment in pediatric Graves’ disease (GD) patients were lower in the remission group. And time to TBII normalization after ATD treatment was shorter in the remission group. Therefore, measurement of TBII level during ATD treatment can be used to predict remission in pediatric GD patients.

Introduction

Hyperthyroidism is a disease associated with clinical symptoms such as goiter and ophthalmopathy due to excessive production of thyroid hormones. The most common cause of hyperthyroidism in children is Graves' disease (GD), accounting for approximately 95% of cases in Korea [1]. GD is caused by organ-specific autoimmunity associated with thyroid-stimulating hormone (TSH) receptor-stimulating antibodies and is linked to genetic predisposition and environmental factors [2,3]. Stimulation of the thyroid gland due to autoimmunity causes follicular cell hypertrophy and an increase in the number of follicular cells, resulting in increased production of thyroid hormones, diffuse goiter, and ophthalmopathy [4].
GD treatment aims to maintain normal thyroid function and prevent hyperthyroidism recurrence. However, the optimal GD treatment in children is controversial. Pediatric GD treatments include antithyroid drug (ATD) treatment, which suppresses thyroid hormone production, and ablative treatments (i.e., radioiodine therapy or surgery). ATDs are primarily used as an initial treatment in children because they are convenient and have the advantage of preventing permanent hypothyroidism, while ablative therapy is considered in cases of hyperthyroid relapse. However, the rate of GD remission with ATD treatment alone is low. In addition, clinical guidelines regarding the timing of ATD treatment discontinuation in children and adolescents have not been established. Hence, we investigated the remission rate following ATD treatment in pediatric patients with GD. We also determined the predictive factors for GD remission.

Materials and methods

1. Subjects

We retrospectively analyzed the clinical data from 98 children and adolescents diagnosed with GD (22 boys and 76 girls) who were followed for more than 5 years at Ajou University Hospital between March 2003 and July 2020. All participants were younger than 18 years at the time of diagnosis and showed evidence of autoimmune disease. ATD treatment was initiated in all patients after being diagnosed with GD based on medical history, clinical symptoms, examination findings (tachycardia, weight loss, increased sweating, goiter, and ophthalmopathy), thyroid function test results, and thyroid autoantibody test results.

2. Patient evaluation and outcome measures

Age, sex, height, weight, body mass index (BMI), pubertal status, pulse rate (tachycardia: pulse rate≥90 BPM), goiter or ophthalmopathy, and family history of thyroid disease were investigated upon initial GD diagnosis. BMI (kg/m2) was calculated from the weight and square of the height, and the BMI standard deviation score (SDS) was calculated using data from the 2007 Korean National Growth Chart [5]. Pubertal development was determined according to Tanner stage (prepuberty vs. puberty) based on breast development associated with a sexual maturity rating ≥2 for females and testicular enlargement to at least 4 mL in volume for males. Goiter was classified using the World Health Organization criteria: grade 0, no goiter; grade 1, mild goiter; and grade 2, severe goiter [6]. At the time of first diagnosis, thyroid function tests were performed by measuring total triiodothyronine (T3), free thyroxine (fT4), and TSH serum levels using immunoradiometric assays (Immunotech s.r.o., Praha, Czech Republic). Tests were performed every 2–4 weeks until thyroid function normalized and every 2–3 months thereafter. In addition, levels of thyroid autoantibodies, antithyroglobulin antibodies (ATAs), and antimicrosomal antibodies (AMAs) were measured using radioimmunoassay (Immunoradiometric assay, Cobra II gamma counter, Packard, Conroe, TX, USA). TSH-binding inhibitory immunoglobulin (TBII) level was measured using a radioreceptor assay (TSH Rezak, Medipan Diagnostica, Dahlewitz, Germany; normal range, 0.0–9.0 U/L) before June 2011. After July 2011, TBII level was measured using a TRAK human radioreceptor assay (BRAHMS, Diagnostica AG, Hennigsdorf, Germany; normal range, 0.0–1.5 U/L); a correction formula was used to standardize TRAb levels with a standard range of 0.0–1.5 U/L [7]. After initiating ATD treatment, the interval to euthyroid status and time to TBII normalization were investigated. In addition, complete blood count and liver function tests were performed at intervals of 2–3 months during the dosing period to identify any side effects associated with ATD treatment. After GD diagnosis, the patient was administered 5–7 mg/kg propylthiouracil (PTU) 3 times a day or 0.5–0.7 mg/kg methimazole (MMZ) once a day. ATD treatment was discontinued if normal thyroid function was maintained and TBII level remained normalized for longer than 1 year. Remission was defined as normal thyroid function for at least 12 months after discontinuing ATD treatment. Patients were considered to have relapsed if they tested positive for TBII, showed increased T3 and/or fT4 levels and decreased TSH level, and showed clinical symptoms corresponding to hyperthyroidism that required resumption of ATD treatment during the total follow-up period.

3. Patient assignment

The participants were divided into 2 groups: patients who maintained remission were categorized into the remission group, while those who had persistent disease were categorized into the nonremission group.

4. Statistical analysis

We compared results of the thyroid function tests and thyroid antibody tests (ATA, AMA, and TBII) at the time of diagnosis, at 3 months, and at 1, 2, 3, 4, and 5 years after ATD treatment between patients in the remission and nonremission groups. IBM SPSS Statistics ver. 25.0 (IBM Co., Armonk, NY, USA) was used to perform statistical analyses. Statistical significance of the findings between the remission and nonremission groups was assessed using the Mann-Whitney U-test for continuous variables and the chi-square test for categorical variables. Multiple logistic regression analysis was performed to determine the factors predicting remission, and odds ratios (ORs) and 95% confidence intervals (CIs) were determined. In model 1, the unadjusted OR and 95% CI were calculated using multiple logistic regression without adjusting for confounders. In model 2, the adjusted OR and 95% CI were determined using multiple logistic regression after adjusting for age, sex, and BMI SDS. In model 3, multiple logistic regression analysis was performed to determine the statistical significance between remission and clinical variables of age, sex, BMI SDS, pubertal stage, goiter, exophthalmos, family history of thyroid disease, TBII level, and time to TBII normalization. We performed receiver operating characteristic (ROC) analyses to evaluate the optimal cutoff time for TBII normalization after ATD treatment in predicting remission. Optimal cutoff time was estimated by calculating Youden index (J, maximum [sensitivity+specificity-1]). A P-value of <0.05 was considered statistically significant.

Results

The mean age of the participants was 11.57±3.13 years. Of the total 98 patients, 76 (77.6%) were female and 22 (22.4%) were male. The mean BMI SDS was 0.06±1.01. We observed goiter in 95 participants (stages 1 [67.3%] and 2 [29.6%]) and ophthalmopathy in 47 (47.9%) participants. In total, 32 participants (32.7%) had a family history of thyroid disease. After initiating ATD treatment, the average time to euthyroid status was 0.43±0.43 months, and the average time to TBII normalization was 3.29±2.70 years.
During the 5-year follow-up period, 18 participants (18.3%; 15 females and 3 males) maintained remission without relapse. Table 1 shows the clinical characteristics at diagnosis according to remission. There were no significant differences between the 2 groups with respect to age, sex, or BMI SDS at the time of GD onset. The average time to discontinue ATD treatment in the remission group was 2.94±1.01 years. In the nonremission group, 74 patients could not discontinue ATD treatment and relapse occurred within 5 years in 6 patients (6.2%) after discontinuing ATD treatment.
Changes in thyroid function and thyroid antibody test results in the remission and nonremission groups over 5 years are summarized in Table 2. Regarding the thyroid function test results, fT4 (3.22 mIU/L vs. 3.77 mIU/L, P=0.024), T3 (387.61 mIU/L vs. 400.69 mIU/L, P=0.032), and TSH (0.03 mIU/L vs. 0.14 mIU/L, P=0.034) levels at diagnosis were significantly lower in the remission group than in the nonremission group.
TBII, AMA, and ATA positivity was observed in 100.0%, 74.5%, and 79.6% of participants, respectively. There were no significant differences in ATA or AMA level between the 2 groups over 5 years. However, TBII level at diagnosis (9.37 U/L vs. 18.88 U/L, P=0.002), at 3 months (5.46 U/L vs. 13.09 U/L, P=0.002), and at 1 year (2.42 U/L vs. 7.67 U/L, P=0.002), 2 years (1.76 U/L vs. 2.30 U/L, P≤0.001), 3 years (1.34 U/L vs. 8.39 U/L, P≤0.001), 4 years (1.78 U/L vs. 7.44 U/L, P≤0.001), and 5 years (1.38 U/L vs. 7.01 U/L, P≤0.001) after ATD treatment were significantly lower in the remission group than in the nonremission group. There was no significant difference between the 2 groups in euthyroid status after ATD treatment. However, time to TBII normalization after ATD treatment (1.65 years vs. 3.65 years, P<0.001) was significantly shorter in the remission group than in the nonremission group.
Multiple logistic regression analysis was performed to evaluate the association between remission and factors related to GD, with remission as the dependent variable (Table 3). As one year to TBII normalization (years) increased, OR for remission decreased 0.639 (95% CI, 0.456–0.894) in unadjusted model 1. This relationship remained statistically significant after adjusting for confounding factors in models 2 and 3. The time to TBII normalization (years) showed ORs for remission of 0.608 (95% CI, 0.425–0.870) and 0.596 (95% CI, 0.374–0.951) in models 2 and 3, respectively.
According to the ROC curve analysis to evaluate optimal cutoff time for TBII normalization after ATD treatment in predicting remission, TBII normalization of 2.35 years correlated with remission with an area under the curve of 0.766, 66.3% sensitivity, and 88.9% specificity.

Discussion

In our study on pediatric GD patients, the remission rate was 18.2% with ATD treatment alone during the 5-year follow-up period. In comparison between the remission and nonremission groups, time to TBII normalization was significantly shorter in the remission group than in the nonremission group. In adult GD patients, the remission rate after 1–2 years of ATD treatment is 40%–50% and the recurrence rate is 30%–70% [8]. Magri et al. [9] reported that, during a 5-year follow-up period, approximately 54.1% of adults receiving ATD treatment showed remission and GD recurred in 11.2% of adults. Although the period for ATD treatment has not been established, studies have reported that the 4- and 5-year remission rates following 2 years of pediatric ATD treatment are 25% and 50%, respectively [10,11]. The incidence of relapse is variable, and recurrence occurs in 3%–47% of pediatric GD patients after discontinuing ATD treatment [1,12]. Lee et al. [13] reported that 6.3% of pediatric GD patients achieved remission after 3 years, 16.4% achieved remission after 4 years, 29.4% achieved remission after 5 years, and 55.8% achieved remission after 6 years post-ATD treatment. In the present study, 18 children (18.3%) achieved remission during the 5-year observation period, and medications could not be discontinued in the remaining 74 patients (75.5%) during this period. The relatively small number of subjects and the selection bias inherent to the retrospective study design might explain why the observed remission rate was lower than that observed in other studies. Relapse occurred in 6 of 24 patients (25%) who discontinued ATD treatment during the 5-year follow-up period. Since the remission rate with ATD treatment alone is low, establishing a treatment plan based on reliable predictive factors for remission is warranted.
Several studies have focused on the identification of predictive factors for remission. Glaser et al. [14,15] concluded that a higher BMI SDS, smaller goiter size, lower initial T3 level, and older age were associated with remission. In addition, several other studies proposed that higher AMA level, higher TSH level, and lower ATA level are correlated with remission [16,17]. However, since most of these studies were retrospective and not large-scale or long-term studies, reliable predictive factors for remission in pediatric patients with GD remain controversial. There were no significant differences in sex, age, BMI SDS, goiter size, fT4, T3, ATA, or AMA level between the remission and nonremission groups in this study. However, the remission group had significantly lower TBII level at diagnosis and 3 months and at 1, 2, 3, 4, and 5 years after ATD treatment relative to the nonremission group. We also found that the remission group had a significant positive relationship with shorter time to TBII normalization. Through ROC analysis, we identified that TBII normalization of 2.35 years was predictive of remission in pediatric GD patients after ATD treatment.
TBII measurement is an essential test for GD diagnosis, and TBII levels are estimated based on thyroid-stimulating or blocking antibody levels. Several studies in adults have indicated that TBII levels can predict GD remission [18-20]. In addition, Lee et al. [13] and Gastaldi et al. [7] demonstrated that rapid TBII normalization is significantly correlated with remission in pediatric GD patients. However, Zimmermann-Belsing et al. [21] concluded that TBII level is not an appropriate predictor of remission in GD patients.
Our study has some limitations. First, bias might have been introduced as the same therapeutic agent was not initially used. We used PTU only when thyrotoxicosis symptoms were severe and switched to MMZ when patient thyroid function normalized. After a possible occurrence of PTU-induced hepatitis was observed, MMZ was administered. Second, since the kit used for measuring TBII changed, we used a correction formula to consider different reference ranges. Finally, due to the retrospective cross-sectional design of the study, temporal and causal associations could not be established. Further studies with larger sample sizes and prospective and longitudinal designs are needed to confirm our findings.
In conclusion, the time to TBII normalization after ATD treatment can be used as an important predictive factor for maintenance of remission in pediatric patients with GD. Reliable predictive factors for remission can help determine whether ATD treatment alone is sufficient or if early ablative treatment is needed. Therefore, measurement of TBII level during treatment can help establish a proper treatment plan for each patient.

Notes

Ethical statement

The study design was approved by the Institutional Review Board of Ajou University Hospital (AJIRB-MED-MDB-20-377), and the requirement for written informed consent was waived due to the retrospective nature of the study.

Conflicts of interest

No potential conflict of interest relevant to this article was reported.

Funding

This research received no specific grant from any funding agency in the public, commercial, or not-for-profit sectors.

Table 1.
Clinical characteristics of the study population at the time of diagnosis of Graves’ disease according to the occurrence of remission during the 5-year follow-up period
Characteristic All participants (n=98) Remission (n=18) Nonremission(n=80) P-value
Female sex 76 (77.6) 15 (83.3) 61 (76.3) 0.515
Age (yr) 11.57±3.13 10.41±3.57 11.83±2.98 0.102
BMI SDS 0.06±1.01 -0.66±1.09 -0.36±0.98 0.160
fT4 (ng/dL) 3.67±1.28 3.22±1.49 3.77±1.21 0.024
T3 (ng/dL) 398.29±215.59 387.61±378.07 400.69±162.11 0.032
TSH (μIU/mL) 0.12±0.71 0.03±0.04 0.14±0.78 0.034
ATA (U/mL) 524.91±958.39 460.72±1113.01 539.54±926.99 0.911
AMA (U/mL) 1,828.79±1,837.23 1,772.33±1983.53 1,841.50±1,815.76 0.960
TBII (U/L) 54.71±77.08 31.27±34.08 60.00±83.01 0.089
Puberty 0.865
 Prepubertal 23 (23.5) 5 (27.8) 18 (22.5)
 Tanner IIb, or Testis ≥4 mL 75 (76.5) 13 (72.2) 62 (77.5)
Tachycardia 80 (81.6) 11 (61.1) 69 (86.3) 0.031
Goiter (grade 2) 29 (29.6) 4 (22.2) 25 (31.3) 0.637
Exophthalmos 47 (47.9) 8 (44.4) 39 (48.8) 0.945
Family history of thyroid disease 32 (32.7) 6 (33.3) 26 (32.5) >0.999
Time to euthyroid (mo) 0.43±0.43 0.35±0.26 0.45±0.46 0.609
Time to normal TBII (yr) 3.29±2.70 1.65±1.38 3.65±2.77 <0.001

Values are presented as number (%) of mean±standard deviation.

BMI, body mass index; SDS, standard deviation score; fT4, free thyroxine; T3, triiodothyronine; TSH, thyroid-stimulating hormone; ATA, antithyroglobulin antibody; AMA, antimicrosomal antibody; TBII, thyroid-stimulating hormone-binding inhibitory immunoglobulin.

Table 2.
Changes in the levels of serum free thyroxine, triiodothyronine, thyroid-stimulating hormone, and thyroid-stimulating hormone-binding inhibitory immunoglobulin during the 5-year follow-up period according to the remission or nonremission of Graves’ disease
Variable Remission Nonremission P-value
At diagnosis
 fT4 (ng/dL) 3.22±1.49 3.77±1.21 0.024
 T3 (ng/dL) 387.61±378.07 400.69±162.11 0.032
 TSH (μIU/mL) 0.03±0.04 0.14±0.78 0.034
 TBII (U/L) 9.37±8.87 18.88±19.30 0.002
At 3 months
 fT4 (ng/dL) 1.35±0.66 1.42±0.69 0.653
 T3 (ng/dL) 135.56±40.00 159.43±60.77 0.143
 TSH (μIU/mL) 5.66±12.39 2.59±9.41 0.872
 TBII (U/L) 5.46±7.41 13.09±8.87 0.002
At 1 year
 fT4 (ng/dL) 1.21±0.24 1.39±0.50 0.102
 T3 (ng/dL) 143.61±36.94 145.35±46.98 1.000
 TSH (μIU/mL) 1.98±0.46 2.96±5.27 0.483
 TBII (U/L) 2.42±4.41 7.67±11.59 0.002
At 2 years
 fT4 (ng/dL) 1.22±0.35 1.37±0.44 0.265
 T3 (ng/dL) 126.17±34.68 133.69±22.28 0.916
 TSH (μIU/mL) 4.79±8.18 2.05±2.51 0.025
 TBII (U/L) 1.76±7.05 2.30±11.26 <0.001
At 3 years
 fT4 (ng/dL) 1.24±0.25 6.86±46.55 0.095
 T3 (ng/dL) 122.53±17.89 148.73±76.91 0.599
 TSH (μIU/mL) 2.70±3.03 2.23±6.04 0.160
 TBII (U/L) 1.34±1.98 8.39±11.48 <0.001
At 4 years
 fT4 (ng/dL) 1.37±0.24 1.53±0.68 0.773
 T3 (ng/dL) 125.83±31.28 143.96±70.05 0.460
 TSH (μIU/mL) 0.96±0.72 1.79±2.65 0.755
 TBII (U/L) 1.78±2.61 7.44±10.83 <0.001
At 5 years
 fT4 (ng/dL) 1.31±0.20 1.56±0.63 0.118
 T3 (ng/dL) 120.33±33.14 141.46±72.40 0.317
 TSH (μIU/mL) 1.44±1.41 1.52±1.84 0.302
 TBII (U/L) 1.38±2.11 7.01±10.72 <0.001
Time to euthyroid (mo) 0.35±0.26 0.45±0.46 0.605
Time to normal TBII (yr) 1.65±1.38 3.65±2.77 <0.001

Values are presented as mean±standard deviation.

fT4, free thyroxine; T3, triiodothyronine; TSH, thyroid-stimulating hormone; TBII, thyroid-stimulating hormone-binding inhibitory immunoglobulin.

Table 3.
Multiple logistic regression analysis of association between remission and clinical variables
TBII OR (95% CI)
Mode 1 Mode 2 Mode 3
At diagnosis (U/L) 0.953 (0.906–1.001) 0.946 (0.896–0.998) 0.990 (0.902–1.086)
3 Months (U/L) 0.922 (0.853–0.995) 0.985 (0.971–0.998) 0.959 (0.798–1.152)
1 Year (U/L) 0.828 (0.680–1.010) 0.819 (0.671–1.001) 1.024 (0.860–1.219)
2 Years (U/L) 0.848 (0.687–1.048) 0.838 (0.674–1.040) 0.927 (0.686–1.252)
3 Years (U/L) 0.711 (0.509–0.993) 0.677 (0.472–0.972) 0.815 (0.576–1.154)
4 Years (U/L) 0.812 (0.653–1.008) 0.806 (0.647–1.003) 0.902 (0.634–1.282)
5 Years (U/L) 0.757 (0.569–1.007) 0.749 (0.563–0.997) 0.949 (0.653–1.379)
Time to normal TBII (yr) 0.639 (0.456–0.894) 0.608 (0.425–0.870) 0.596 (0.374–0.951)

OR, odds ratio; CI, confidence interval; TBII, thyroid- stimulating hormone-binding inhibitory immunoglobulin.

Model 1: Statistical significance between remission and clinical variables was determined using multiple logistic regression with no adjustments. Model 2: Statistical significance between remission and clinical variables was determined using multiple logistic regression after adjusting for age, sex, and body mass index (BMI) standard deviation score (SDS). Model 3: Statistical significance between remission and clinical variables, including age, sex, BMI SDS, pubertal stage, goiter, exophthalmos, family history of thyroid disease, TBII levels, and time to TBII normalization was determined using multiple logistic regression analysis.

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