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Thyroid hormones are essential for the development of the central nervous system early in life. Congenital hypothyroidism once caused the devastating cognitive and physical deficits of cretinism, but this condition is now detected routinely at birth using population-wide neonatal screening in most countries. Early and continuous treatment of these children with levothyroxine (LT4), according to age-specific reference ranges, ensures near-normal neuropsychological development, with preserved IQ, although the possibility of subtle residual effects on some indices of neuropsychological functioning remain an active area of research. Children who develop overt hypothyroidism also require treatment with LT4. Most children diagnosed with subclinical hypothyroidism are unlikely to require intervention with LT4, as this condition reverses spontaneously over time. These children should be monitored for possible deterioration of thyroid function in future, especially where thyroid autoimmunity is present.
1 Introduction
This chapter considers the aetiology, clinical course, and management of hypothyroidism in children. Thyroid hormones are essential for normal physical and neural development in neonates, and many countries include a measurement of thyrotropin (thyroid-stimulating hormone; TSH) in their neonatal screening programmes.
The genetic control of thyroid hormone levels appears to function similarly in children and adults [1]. Levels of thyroid hormones differ markedly with age, however. The average level of thyrotropin is high, and highly variable, compared with usual adult measurements [2, 3]. One study showed that the average thyrotropin (thyroid-stimulating hormone, TSH) level was 6.4 mIU/L at birth, declining to 5.5, 6.6, 3.8, 2.9, and 2.1 mIU/L at 1, 2, 3, 4, and 7 days after birth, respectively [2]. Fig. 1 shows average levels of thyroid hormones from 1 month to 18 years of age [3].
Determination of reference ranges for thyroid hormones in other populations of children have confirmed the different evolution of levels of these hormones in children, compared with adults [4, 5]. These data emphasise the importance of using age-appropriate reference ranges for the diagnosis of thyroid dysfunction [5]. In general, a TSH level >5 mIU/L may be considered abnormal in children older than 1 month.
2 Overview of Hypothyroidism in Children
2.1 Congenital Hypothyroidism
The recognition of the causative role of severe, untreated hypothyroidism in the disastrous neurodevelopmental damage associated with cretinism was an important milestone in the historical development of the field of thyroidology (see chapter, “Therapeutic Use of Levothyroxine: A Historical Perspective” of this book). However, hypothyroidism may be transient in newborns identified via neonatal screening, especially when the initial TSH level is mildly elevated at diagnosis, or when relatively low LT4 doses are required for the first 2 years of life [6]. Children with congenital hypothyroidism appear to be at increased genetic risk of other adverse outcomes, including other congenital defects [7], non-alcoholic fatty liver disease [8], or urinary tract disorders [9], compared with the general population.
The optimal TSH cut-off level to diagnose congenital hypothyroidism is still a matter of debate. A study from the USA showed that TSH levels only slightly outside the reference range (e.g. ~5 mIU/L) were a poor predictor of future thyroid dysfunction, and such children need not be referred for specialist care and possible treatment [10]. However, another research group calculated that a TSH cut-off value of 6 mIU/L was optimal for identifying congenital hypothyroidism (transient or permanent) that may have required treatment [11].
2.2 Subclinical Hypothyroidism
2.2.1 Prevalence and Clinical Course
The prevalence of subclinical hypothyroidism in paediatric subjects is reported as being <2%, generally lower than the prevalence of this condition in adults [12, 13]. A large database analysis, conducted using records of more than 1 million paediatric outpatients, found that TSH was 5.5–10 mIU/L in 2.9%, and >10 mIU/L in 0.4% [14]. A recent study of more than 3 million children in Italy using administrative health databases for the years 2001–2014 found an annual prevalence of subclinical hypothyroidism (based on receipt of a low dose of LT4) of 1 case per 5000 children [15]. The annual prevalence remained relatively stable over time and tended to increase at age >10 years.
Many children with subclinical hypothyroidism revert to normal thyroid function or, at least, do not deteriorate to overt hypothyroidism [14, 16]. The analysis of >1 million children revealed that TSH reverted to within the normal range in 76% of children with initial 5.5–10 mIU/L, and in 40% of those with initial TSH >10 mIU/L [14]. The presence of thyroid autoimmunity, or higher levels of TSH at baseline, predicts a more severe clinical course, however [16,17,18,19,20]. In one study, the presence of Hashimoto’s thyroiditis with high titres of anti-thyroglobulin antibodies was associated with a 28-fold higher risk of needing LT4 treatment vs. Hashimoto’s thyroiditis patients without the presence of these antibodies [17]. Elsewhere, 63% of a population of girls with Hashimoto’s thyroiditis and subclinical hypothyroidism required LT4 treatment during 5 years of follow-up, compared with 24% of girls without autoimmunity; the proportions with overt hypothyroidism at 5 years were 31% (with thyroid autoimmunity) and 12% (without thyroid autoimmunity) [21]. Children with Hashimoto’s thyroiditis may still recover normal thyroid function, as shown by a study which involved withdrawal of LT4 therapy from 148 children or adolescents with this condition. One third of the population did not need re-initiation of LT4 after 2 years off-treatment [22].
2.2.2 Outcomes in Children with Subclinical Hypothyroidism
Subclinical hypothyroidism is associated with obesity in paediatric subjects [23, 24]. A retrospective study identified subclinical hypothyroidism (normal FT4, TSH 5–10 mIU/L) in 36% of a population of 215 obese children and adolescents [25]. Subjects with vs. without subclinical hypothyroidism were more insulin resistant and showed signs of atherogenic dyslipidaemia (low HDL-C, high triglycerides), but BMI was similar. Waist, BMI, LDL-C, serum triglycerides, and a measure of insulin resistance were higher, and HDL-C was lower, in 27 children (mean age 11 years) with subclinical hypothyroidism, compared with a control group [26]. Other studies have associated subclinical hypothyroidism with high blood pressure and/or other components of the metabolic syndrome in children or adolescents [23, 24, 27,28,29]. The TSH level correlates with insulin resistance or triglycerides in euthyroid children, also [30].
A study in 32 children with autoimmune thyroiditis and subclinical hypothyroidism (mean age 14 years) revealed increased atherogenic index, a greater thickness of epicardial fat (an emerging risk factor for metabolic dysfunction), and reduced endothelial vascular function, compared with 32 healthy matched control children [31]. A further study in 64 children also associated subclinical hypothyroidism with dyslipidaemia and increased cIMT vs. controls, although upper diagnostic limit for TSH was 20 mIU/L, and may have included children with overt hypothyroidism [32]. However, another observational study, in 110 obese children, found no correlation between TSH level and dyslipidaemia or carotid intima-media thickness, a measure of the overall burden of atherosclerosis [33].
Relatively mild neuropsychological deficits have been observed in children with subclinical hypothyroidism, relating mainly to indices of attention [12, 34, 35], or verbal memory/verbal recall [36]. Measures of intelligence of cognition were generally unaffected in these studies.
Finally, no impairment of growth or bone maturation was observed in a population of 36 children with persistent, untreated subclinical hypothyroidism followed for an average of 3.3 years [37].
2.3 Other Causes of Hypothyroidism in Children
Several other factors can produce a hypothyroid-like state in children, including consumptive hypothyroidism due to infantile hepatic hemangioma [38], older antiepileptic drugs [39], chronic liver disease [40], or gastrointestinal disorders [41]. Other autoimmune diseases, such as type 1 diabetes or celiac disease tend to cluster with hypothyroidism in children [42,43,44]. Hyperprolactinaemia is also strongly associated with thyroid status: a cross-sectional study of 602 children found this disorder on 32% of children with subclinical hypothyroidism and 52% of children with overt hypothyroidism [45]. Finally, the prevalence of hypothyroidism may be higher in children with Down syndrome or Turner Syndrome, compared with the general population [46,47,48,49,50,51].
Hypothyroidism can also follow partial thyroid resection. A retrospective review of 14 aged <18 years children who had undergone hemithyroidectomy for benign thyroid nodules showed that only one patient in six needed LT4 replacement [52]. The authors suggested that these patients should be followed for sufficient time to allow natural recovery of thyroid function, before administration of LT4.
3 Effects of Levothyroxine in Children with Hypothyroidism
3.1 Congenital or Overt Hypothyroidism
Children with any form of overt hypothyroidism must be treated promptly with LT4 [53]. Treatment for congenital hypothyroidism should start within the first 2 weeks of life, and even before a confirmatory thyroid function test in more severe cases [54, 55]. A recommended starting dose is 10–15 mg/kg/day given orally, with the precise dose depending on the severity of the condition. Early and continuous treatment with LT4 effectively prevents the onset of the gross adverse effects of hypothyroidism in the brain [54]. For example, Fig. 2 shows the similar scores for measures of intelligence quotient (IQ) for children with early- and continuously treated congenital hypothyroidism, compared with euthyroid children in one study [56], and according to initial doses of LT4 in another study [57]. No behavioural abnormalities were observed between groups in the first study [56]. Optimisation of LT4 treatment is important in preserving neuropsychological outcomes in this population, as over- or under-treatment with LT4 early in life has been associated with neuropsychological or behavioural problems later on [56, 58, 59].
Severe hypothyroidism may be associated with subtle and long-lasting neurocognitive deficits, even when children are identified via new born screening and treated promptly with LT4. This was shown in a recent study in 30 such children aged at least 6 years, who demonstrated multiple brain white matter lesions, which correlated with deficits in language development [60]. A study from Turkey showed mild-to-moderate developmental delay at age 2–3 years in early-diagnosed and treated children with congenital hypothyroidism [61]. Ten-year old children with congenital hypothyroidism who were diagnosed via neonatal screening have been shown to be at risk of reduced health-related quality of life (HRQoL), and adverse perception of self-worth, compared with their euthyroid peers [62]. These deficits in QoL were independent of cognitive or neuropsychological functioning.
3.2 Subclinical Hypothyroidism
Individual studies have demonstrated that LT4 treatment reduced hypothyroid-like symptoms in children with subclinical hypothyroidism [63], or the mean anti-thyroglobulin titre in children with Hashimoto’s thyroiditis [64]. Treatment of children with mild, subclinical hypothyroidism with LT4 was not disease modifying, in that it did not decrease the likelihood of an increase in TSH after treatment withdrawal [65]. There is little evidence to support improved neuropsychological outcomes with LT4 treatment in this population, however [34]. One prospective study found significantly reduced scores for verbal memory and verbal recall in 20 children with TSH 5–10 μIU/L, compared with a control group [36]. Treatment for 6 months with LT4 restored the test performance in the children with subclinical hypothyroidism to the level of controls.
Obesity is associated with hypothyroidism (especially the subclinical form) in children, as described above. A 6-month, randomised trial in 51 obese children with TSH 4–10 mIU/L (with or without abnormalities of other thyroid hormones) showed that administration of LT4 vs. no additional treatment, alongside weight loss interventions, had no significant effect on BMI or lipid abnormalities [66]. A similar study, where LT4 was or was not added to a behavioural intervention for obesity, reported similar results [67]. These data suggest there is no place for LT4 in the general management of obesity in children with TSH levels consistent with subclinical hypothyroidism. Correlations of higher TSH levels with higher BMI in hypothyroid children controlled on LT4 have been observed [68], but this association is probably not independently causative for obesity [1, 69].
Administration of LT4 to 30 children with subclinical hypothyroidism (mean age 7 years, mean TSH 8.7 mIU/L) for 6 months increased measures of left ventricular systolic performance (myocardial performance index, fraction shortening, and ejection fraction), but did not affect diastolic function (E/E′ ratio) [70]. This study was uncontrolled, and these parameters were not overtly decreased before treatment, so that the clinical relevance of these findings is difficult to assess. Migraine may be a symptom of subclinical hypothyroidism, which responds to treatment with LT4 [71].
Box 1 summarises guideline recommendations for the management of subclinical hypothyroidism in children [43, 53, 69]. The majority of this population will not need active treatment, as long as thyroid hormones are within range and thyroid function is not deteriorating. The European guidance differs from the guidelines from Latin America and from the USA since it was specifically addressed for hypothyroidism in children, and it identifies the first 3 years of life as the crucial period for optimising thyroid function with LT4 (this is the time when thyroid hormones have their greatest influence on development of the brain). Monotherapy with LT4 is used exclusively: there is no role for the therapeutic use of T3 currently, as in other populations. A recent expert opinion recommends reserving LT4-based management of subclinical hypothyroidism to children with autoimmune (Hashimoto) disease, children whose thyroid function is deteriorating over time, or for children with goitre, other congenital abnormalities associated with thyroid dysfunction (Turner Syndrome or Down Syndrome) [72].
Box 1: Summary of Guidance Relating to the Use of Levothyroxine (LT4) in Children with Subclinical Hypothyroidism [46, 53, 69]
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Discuss decisions to treat or not to treat with LT4 carefully with parents/guardians
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Most children with TSH <10 mIU/L and FT4 or TT4 within normal range will not need treatment with LT4
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Initiating LT4 is a reasonable strategy for patients with TSH >10 mIU/L, including children
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Especially beyond 1 month of age and who have signs and symptoms of hypothyroidism and/or risk factors for progression of thyroid dysfunction
-
-
Use LT4 only, there is no current role for treatment with LT3
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Consider a trial of withdrawal of LT4 at age 3 years, as development of the CNS is no longer dependent on thyroid function
-
Monitor the TSH level and for thyroid autoimmunity periodically beyond age 3 years (more frequent monitoring is recommended if thyroid autoimmunity is present already)
Guidance has been adapted and combined from Latin American [46], the USA [53], and European [69] guidelines and has been paraphrased for brevity. See the full guidelines for more details
3.3 Biochemically Euthyroid Children
A randomised trial in 59 biochemically euthyroid children with Hashimoto’s thyroiditis showed that treatment with LT4 (mean dose 1.6 μg/kg/day, based individually on body weight) vs. no treatment reduced thyroid volume transiently, and did not affect either thyroid function or the level of thyroid autoantibodies [73]. Observational data from 330 children with autoimmune thyroiditis and type 1 diabetes showed a reduction in antibodies in the treated cohort, suggesting a possible role for LT4 therapy in this population [74].
4 Conclusions
Thyroid hormones are essential for the development of the central nervous system early in life. Early and continuous treatment with LT4 of children with overt hypothyroidism preserves near-normal neuropsychological development. Subclinical hypothyroidism often resolves spontaneously and most children will not need LT4 treatment. However, close observation is key since some children with this condition may require LT4 to manage symptoms, or they may develop overt hypothyroidism in the future.
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Brenta, G. (2021). Levothyroxine in Children. In: Kahaly, G.J. (eds) 70 Years of Levothyroxine. Springer, Cham. https://doi.org/10.1007/978-3-030-63277-9_5
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DOI: https://doi.org/10.1007/978-3-030-63277-9_5
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