Background
Fetal hyperthyroidism usually occurs in the second and third trimesters of pregnancy. Neonatal hyperthyroidism tends to be an extension of disease sustained in utero; it is harmful in the fetal and neonatal periods and requires guideline-directed clinical management. Most neonatal hyperthyroidism is transient, commonly caused by stimulation by maternal thyroid-stimulating hormone receptor antibody (TRAb) crossing the placenta, resulting in a baby’s high thyroid hormone secretion. In rare situations, thyroid disease is associated with a genetic variation in the thyroid-stimulating hormone receptor (TSHR) or G-protein alpha stimulatory subunit (GNAS) gene such as in McCune-Albright syndrome [1].
The prevalence of neonatal hyperthyroidism is 1 in 25,000 newborns to 1 in 50,000 newborns [1]. The most severe hazard in utero is prolonged tachycardia, leading to increased cardiac output, cardiac failure, and even intrauterine fetal demise. The clinical manifestations in the neonatal period are tachycardia, irritability, hyperphagia without weight gain, goiter, thyroid eye disease, small anterior fontanel, advanced bone age, hepatomegaly, and/or splenomegaly. Severely affected patients could present with cardiac failure, craniosynostosis, microcephaly, psychomotor disabilities, and even death [2]. TRAb levels should be measured in cord blood at delivery; nearly one-third of infants with increased cord blood TRAb levels develop neonatal hyperthyroidism. A newborn with such symptoms should receive timely medical intervention. If timely diagnosis and proper treatment are obtained, the prognosis of most patients is favorable. Consequently, clinicians need to monitor maternal and fetal thyroid function.
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In this study, we revisit a case of a newborn child with a perinatal history of maternal thyroid disorder.
Case presentation
The 31-year-old mother had hyperthyroidism five years prior and took oral methimazole accordingly; however, the mother’s TRAb remained stable at over 40 IU/ml, refractory to treatment. She had undergone a spontaneous abortion three years prior and consequently underwent subtotal thyroidectomy one year prior to control the thyroid function. She regularly took levothyroxine sodium (LT4) postoperatively, and the patient was assessed to have normal thyroid function with elevating TRAb concentration from pre-gestation (T3 1.99 nmol/L, fT3 5.10 pmol/L, T4 145.5 nmol/L, fT4 17.83 pmol/L, TSH 0.58 μIU/ml, TRAb > 40 IU/ml) to the second trimesters of pregnancy (> 40 IU/ml). However, at 32 weeks of gestation, the fetal heart rate increased to 172 beats per minute, persistent for over 10 min during the electronic fetal monitoring, and thyroid ultrasound revealed fetal goiter with decreased echo. The mother The dimensions of the fetal thyroid were 75.2 mm. The obstetrician suggested withdrawing levothyroxine and introducing methimazole at a dose of 15 mg per day. In the latter part of pregnancy, we arranged pregnancy check-ups weekly. Close fetal heart rate monitoring fluctuated between 140 and 160 beats per minute. The fetal ultrasound showed neither hydrops fetalis nor cardiac hemodynamic changes. The multi-disciplinary team proposed initiating a therapeutic trial that involved concurrently administering methimazole 15 mg and levothyroxine sodium 125 μg until delivery. We monitored maternal heart rate, complete blood count, and liver function and advised adding metoprolol if necessary. The indicators above are normal, and the patient had no associated symptoms. The details of the laboratory tests of thyroid function are listed in Table 1.
Table 1
Thyroid function tests of the mother before and during pregnancy
Gestation weeks | Bodyweight (kg) | T3 nmol/L | fT3 pmol/L | T4 nmol/L | fT4 pmol/L | TSH μIU/ml | TRAb IU/ml | Treatment | |
|---|---|---|---|---|---|---|---|---|---|
LT4(μg) | Methimazole (mg) | ||||||||
Pre-gestation | 53.4 | 1.99 | 5.10 | 145.5 | 17.83 | 0.58 | > 40 | 50 | / |
1+ 2 | / | 2.12 | 5.26 | 134.5 | 19.46 | 0.75 | / | 50 | / |
4+ 2 | / | 1.66 | 4.56 | 138.71 | 12.71 | 2.40 | / | 75 | / |
6+ 6 | / | 2.26 | 5.27 | 168 | 20.53 | 0.66 | / | 62.5 | / |
9+ 6 | / | / | / | / | 17.55 | 0.14 | / | 62.5 | / |
13+ 1 | / | 3.22 | 5.30 | 238.2 | 21.28 | 0.04 | / | 50 | / |
16+ 6 | / | 3.01 | 4.98 | 243.5 | 18.04 | 0.04 | / | 25 | / |
20+ 2 | 58.8 | 3.11 | 4.01 | 162.5 | 13.92 | 3.04 | 39.46 | 25 × 4d + 50 × d | / |
23+ 2 | / | 2.54 | 3.70 | 138 | 13.06 | 4.39 | / | 50 × 5d + 75 × 2d | / |
26+ 2 | 65 | 3.56 | 4.79 | 193 | 15.96 | 0.49 | / | 50 | / |
30+ 2 | 66.2 | 3.58 | 5.03 | 232.9 | 17.04 | 0.13 | > 40 | 25 | / |
32+ 2 (fetus goiter) | 67.3 | 3.03 | 4.89 | 205.2 | 16.35 | 0.2 | / | Withdrawal | / |
33 | / | / | / | / | / | / | / | / | 15 |
34+ 1 | 68.4 | 2.31 | 3.65 | 144.1 | 13.91 | 1.82 | / | 50 | 10/5 alternating |
35+ 1 | 68.9 | 2.27 | 3.52 | 128.3 | 10.08 | 6.35 | / | 75 | 10/5 alternating |
36 | 70.5 | 2.49 | 3.85 | 146.7 | 11.76 | 15.02 | 86.3 | 125 | 15 |
37 | 69.8 | 2.71 | 4.31 | 170.9 | 15.57 | 4.16 | / | 125 | 15 |
38 | 70 | 2.64 | 4.31 | 232.4 | 16.69 | 1.08 | / | 125 | 15 |
A male neonate, appropriate for gestational age, was born by vaginal delivery at 37 weeks and five days with a weight of 3130 g. The newborn had no fetal distress, no maternal history of premature rupture of membranes, or neonatal asphyxia. At birth, the placenta and appendages were normal. The primary reason for hospitalization was a thyroid disorder since the gestational age of 32 weeks. Upon delivery, the child’s physical examination revealed stable vital signs, irritability, small anterior fontanel, proptosis, enlarged cardiac borders on percussion, and normal heart rate for age. The main objective of hospitalization was evaluating the primary disease and its complications.
We actively carried out relevant laboratory tests and targeted treatments for thyroid disorders. The umbilical arterial thyroid function test showed triiodothyronine (T3) 1.36 nmol/L (0.49–3.30 nmol/L), free triiodothyronine (fT3) 3.15 pmol/L (3.50–6.50 pmol/L), thyroxine (T4) 145.5 nmol/L (151.9–198.6 nmol/L), free thyroxine (fT4) 19.04 pmol/L (11.48–22.70 pmol/L), thyroid-stimulating hormone (TSH) 0.01 μIU/ml (1.10–19.12 μIU/ml). The serum anti-thyroglobulin antibodies (TgAb; 16.71 IU/ml) were noted, and TRAb exceeded 40 IU/ml. The thyroid ultrasound revealed an enlarged thyroid gland, and the width of the left lobe, right lobe, and isthmus of the thyroid gland was 1.1 cm, 1.2 cm, and 0.3 cm, respectively. The initial chest radiograph suggested cardiac enlargement; however, myocardial enzymes and B-type natriuretic peptide were within normal ranges. The ultrasonic cardiogram on day two showed patent ductus arteriosus (5.1 mm × 2.1 mm), and an average left ventricular ejection fraction (74%). Holter monitoring showed a heart rate of 140–200 beats per minute for 36% of the day. On the third day of life, the patient was started on a 0.4 mg of oral methimazole regimen every 12 h, at 0.25 mg/kg/day. On day seven, the patient was administered propranolol 0.5 mg every 8 h. We subsequently achieved reasonable control of the heart rate. During hospitalization, we regularly monitored thyroid function tests and TRAb levels. There was a gradual downward trend on T4, while the T3, fT3, and fT4 had no evident changes. The patient’s condition was deemed stable; meanwhile, the substantial value of TRAb was assayed for the first time before discharge. He was subsequently discharged for further outpatient follow-ups. On the 29th day of life, the TRAb level fell to 23.13 IU/ml for the first time in the patient’s clinical course. On the 51st day of life, the gradually diminishing T4, fT4, and TRAb (10.96 IU/ml) levels combined with recovering TSH levels (0.53μIU/ml) prompted us to halve the dosage of methimazole (0.125 mg/kg). On the 88th day of life, the follow-up studies showed the thyroid function test and TRAb level. Eventually, on day 98, the neonatologist discontinued all medications onboard. Meanwhile, the patient underwent a developmental assessment on routine follow-ups, appropriate for age. Details of thyroid function tests are summarized in Table 2.
Table 2
Thyroid function tests over the first 88 days of the infant’s life
Date | T3 nmol/L | fT3 pmol/L | T4 nmol/L | fT4 pmol/L | TSH μIU/ml | TRAb IU/ml | Treatment |
|---|---|---|---|---|---|---|---|
Day 0 | 1.36 | 3.15 | 145.5 | 19.04 | 0.01 | > 40 | |
Day 2 | 2.46 | 6.49 | 183.6 | 23.46 | 0.01 | > 40 | methimazole 0.25 mg/kg/day on Day 3 |
Day 5 | 2.5 | 5.28 | 188.6 | 19.77 | 0.01 | ↓ | |
Day 11 | 3.0 | 7.26 | 151.8 | 20.62 | 0.01 | 65 (diluted) | ↓ |
Day 29 | 3.5 | 8.8 | 115.9 | 17.58 | 0.01 | 23.13 | ↓ |
Day 51 | 2.07 | 4.69 | 73.7 | 10.18 | 0.53 | 10.96 | methimazole 0.125 mg/kg/day |
Day 58 | 2.01 | 4.29 | 64.4 | 8.7 | 2.51 | / | ↓ |
Day 88 | 3.1 | 8.05 | 128 | 19.24 | 0.11 | 3.87 | withdrawal |
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Discussion and conclusion
Previous studies have shown that untreated or even partially treated overt hyperthyroidism during pregnancy could increase the risk of pregnancy loss and fetal mortality [3, 4]. Women diagnosed with hyperthyroidism should counsel the endocrinologist regarding plans for pregnancy and the adverse effects of both antithyroid drugs and LT4 during pregnancy [5]. Some studies showed that treatment with surgery before pregnancy is recommended for those who desire future pregnancy with a high TRAb level [6‐8]. If surgery is undertaken, hypothyroidism should be treated with levothyroxine to achieve a euthyroid state before trying to conceive. Next, according to the guideline by American Thyroid Association in 2017, a maternal serum determination of TRAb is recommended at initial thyroid function testing during early pregnancy among all women with a prior history of hyperthyroidism treated with surgery [9, 10].
In this case, the mother underwent a prior miscarriage due to thyroid disorder. She underwent surgery to prevent fetal and neonatal thyroid disorder. However, the stubborn elevating TRAb level at a critical stage of pregnancy resulted in fetal and neonatal hyperthyroidism and tachycardia. Considering the risk of intrauterine growth restriction, fetal bradycardia, and neonatal hypoglycemia, [11] the obstetrics and gynecology team decided against maternal administration of propranolol. It is worth noting that there is a subtle balance between maternal TRAb and thyroid hormones. The complicated regulation of maternal thyroid function is a rigorous challenge for medical intervention. Despite thyroidectomy to avoid miscarriage, the human body still secretes TRAb, which crosses transplacentally to enter the fetal circulation, resulting in hyperthyroidism during the fetal and neonatal periods. Taking ATDs could inhibit the synthesis of T3 and T4. Meanwhile, levothyroxine could protect against resultant hypothyroidism.
In this therapeutic dilemma of maternal hypothyroidism with secondary fetal hyperthyroidism, medical procedures should focus on (1) regular thyroid function screening during pregnancy. The diagnostic criteria for maternal hyperthyroidism include goiter, tachycardia (> 120 beats per minute), ophthalmopathy, and weight loss. The key laboratory finding is the thyroid function test, primarily T3, TSH, and TRAb titers [9]. (2) For women with hyperthyroidism who had previously been treated with radioactive iodine, surgery, or taking oral ATD, serum TRAb was recommended to detect in the first trimester of pregnancy. If serum TRAb is negative early in pregnancy, retesting is not required. If the result presents an elevating TRAb, retesting at 18 to 22 weeks of gestation is recommended. Serum TRAb should be tested again during the third trimester and evaluate the need for fetal and neonatal monitoring on the condition that the repeated measurement is elevated or ATD is initiated [12]. Combining the guideline in China with the clinical situations of our pregnant mother, we designed a meticulous scheme to facilitate clinical decision-making [13]. Once maternal thyroid function disorder is biochemically detected, medications are subsequently titrated to maintain a stable thyroid function for an asymptomatic status. Based on keeping normal thyroid function of the mother, clinicians should pay more attention to reasonable stability of fetal condition, including maintaining normal thyroid appearance, regional blood flow, in utero growth, and fetal heart rate. The fetus should be monitored every 4–6 weeks from mid-pregnancy until birth [14]. According to this case experience, the level of thyroid function is not parallel with the TRAb. The general treatment principle is to maintain a constant maternal thyroid function, reducing fetal complications. The goal is to prepare for the transition to neonatal treatment. (3) Hyperthyroidism patients with good antithyroid drug adherence have a lower risk of severe complications [15]. The adherence of pregnant women to therapy is of primary importance. There is no consensus on the best practice for the dosage of ATD, and the treatments are empirical. According to the condition of pregnant women and the degree of fetal goiter, the multi-disciplinary team should draw up an individual schedule. The lowest effective dose may be applied during the therapy of fetal hyperthyroidism to minimize the risk of fetal hypothyroidism. Maintaining maternal serum fT4 levels at or moderately above the upper limit of the reference range is appropriate for euthyroid fetal status.
In summary, thyroid disorders are one of the main topics in pregnancy complications. At present, more attention has been paid to the effects of hormone abnormalities on infertility, pregnancy outcomes, and long-term motor and intellectual development in offspring. Maternal and fetal diseases identification has gradually improved with the development of endocrinology, perinatology, obstetrics and gynecology, fetal medicine, pediatrics, genetics, and ultrasonic medicine. The multi-disciplinary team makes it possible to manage both maternal and fetal/neonatal thyroid disease from the prenatal period to post-delivery. For a mother with subtotal thyroidectomy, the maternal body may be in a state of hypothyroidism and high-level serum TRAb. It is challenging for clinical decisions to decrease the serum level. Identifying and managing fetal/neonatal thyroid diseases at an early stage of life and reducing long-term comorbidities are crucial issues that need to be solved. Therefore, monitoring fetal surveillance and dosage adjustment to relieve the symptomatic fetal effect without deteriorating the mom is critical.
Acknowledgments
The authors wish to express their gratitude to the patient and his family. The authors would like to thank Editage (www.editage.cn) for English language editing.
Declarations
Ethics approval and consent to participate
This case report was approved by the Ethics Committee of the Peking University First Hospital (2021–175).
Consent for publication
Written informed consent for publication of this case report was obtained from the mother for herself and the newborn child.
Competing interests
The authors declare that they have no competing interests.
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