Hyperthyroidism during pregnancy is uncommon, affecting approximately 1 in 500 pregnancies 1. Overt hyperthyroidism has well-documented adverse impacts on pregnancy outcomes, such as preterm birth, congenital anomalies and pre-eclampsia 2–4. Therefore, despite its rarity, proper management of hyperthyroidism during pregnancy is of utmost importance. Medical therapy is preferred by most authorities because radioiodine is contra-indicated and because thyroidectomy requires pre-treatment with antithyroid drugs and may be complicated by surgical adverse effects 5. The available antithyroid drugs (ATDs) are propylthiouracil (PTU) and methimazole (MMI)/carbimazole (CZ). These drugs are equivalent in terms of their efficacy for the treatment of clinical hyperthyroidism 6. Concerning hyperthyroidism during pregnancy, some reports suggest an association between a specific congenital malformation (MMI embryopathy) and prenatal exposure to MMI 7. The specific malformation pattern related to prenatal MMI exposure consists of choanal and esophageal atresia, scalp defects, minor facial anomalies and psychomotor delay 8. The reported facial anomalies typically include upward slanted palpebral fissures, arched flared eyebrows and a small nose with a broad bridge 9. A recent study conducted by Anderson et al. demonstrated that ventricular septal defect (VSD) is another component of MMI embryopathy 10. Compared with non-exposure, exposure of children to MMI/CMZ during early pregnancy (up to and including gestational week 10) is associated with an increased risk of VSD. PTU may be safer than MMI, and PTU should be considered as the first-line agent for the treatment of hyperthyroidism during pregnancy 11. In contrast, other studies have shown an equal risk of birth defects among pregnant women with hyperthyroidism treated with PTU or with MMI 12, and several major birth defects have been observed in the offspring of women treated with PTU 13. Unilateral kidney agenesis and malformations of the face and neck region have been associated with in utero exposure to PTU. In a case-control study conducted by Clementi et al., PTU exposure was significantly associated with an increased risk of situs inversus, with or without dextrocardia 6. Recent animal studies have demonstrated that PTU is teratogenic during the late blastula, gastrulation and neurulation stages. PTU can alter ciliary-driven flow and can disrupt the normal genetic program involved in left-right axis determination 14. Thus, there is no consensus regarding the best method of therapy for hyperthyroidism during pregnancy. In this study, we evaluated the association of either PTU or MMI treatment for hyperthyroidism during pregnancy with congenital malformations and conducted a systematic review.

Figure 1 shows the selection process after the search. Of the 7 articles included in this systematic review, 6 reported on MMI use, 6 reported on PTU use and 2 reported on shifts between MMI and PTU. The patients in the included studies were pregnant women with hyperthyroidism who required treatment with antithyroid medication to maintain their thyroid hormone levels within the normal range. All controls were pregnant women who either exhibited euthyroidism or presented with hyperthyroidism that was observed late in pregnancy; the latter group of patients delivered before therapy and did not require any antithyroid medication therapy 12. The characteristics of the included articles are reported in Table 1.

Figure 1.

Flow chart of the literature search and article selection.

(0.04MB).

The effect of PTU use on congenital malformations

A total of 7 studies reported on congenital malformations after exposure to PTU. Compared with healthy pregnant women, only one study showed an increased risk of congenital malformations in pregnant women treated with PTU 17. Three other studies did not detect any difference in the congenital malformation rate 13,18,19. A meta-analysis of these four studies concerning the association of exposure to PTU with congenital malformations resulted in a pooled OR of 1.29, with a 95% CI of 1.07–1.55, indicating a mild difference (Figure 2A). We further compared the risk of congenital malformations in pregnant women exposed to PTU with that in women who were not exposed to any ATD during pregnancy. The pregnant women in the non-ATD-exposed group either exhibited euthyroidism throughout pregnancy, thus requiring no medication, or presented with hyperthyroidism that was observed late in pregnancy. The latter group of patients delivered before therapy. There was no statistically significant association between exposure to PTU and the risk of birth defects (pooled OR 1.18, 95% CI 0.97–1.42) (Figure 2B).

Figure 2.

Forest plot of the odds ratios and 95% confidence intervals of the pooled studies. (A) PTU-treated pregnant hyperthyroid women compared with healthy pregnant women according to the risk of congenital anomalies. (B) PTU-treated pregnant hyperthyroid women compared with pregnant hyperthyroid women not receiving any ATD treatment according to the risk of congenital anomalies.

(0.06MB).

The effect of MMI use on congenital malformations

As shown in Figure 3A, six studies reported on congenital malformations after exposure to MMI. Three studies showed an increased risk of congenital malformations in the group of pregnant women treated with MMI compared with the control group 11,17,20. Three other studies did not detect any difference in the congenital malformation rate 12,13,18. A meta-analysis of these six studies concerning the association of exposure to MMI with congenital malformations resulted in a pooled OR of 1.76, with a 95% CI of 1.47–2.10, indicating a significant difference. Even compared with women with hyperthyroidism who were not exposed to any ATD during pregnancy, there was a significantly increased risk of birth defects in women exposed to MMI (pooled OR 1.71, 95% CI 1.39–2.10) (Figure 3B).

Figure 3.

Forest plot of the odds ratios and 95% confidence intervals of the pooled studies. (A) MMI-treated pregnant hyperthyroid women compared with healthy pregnant women according to the risk of congenital anomalies. (B) MMI-treated pregnant hyperthyroid women compared with pregnant hyperthyroid women not receiving any ATD treatment according to the risk of congenital anomalies.

(0.07MB).

The effect of shifts between MMI and PTU use on congenital malformations

As shown in Figure 4, two studies reported on congenital malformations after shifting between MMI and PTU. Both studies showed an increased risk of congenital malformations in pregnant women whose treatment shifted between MMI and PTU compared with the controls 13,17. A meta-analysis of these two studies resulted in a pooled OR of 1.88, with a 95% CI of 1.27–2.77, indicating a significant difference.

Figure 4.

Forest plot of the odds ratios and 95% confidence intervals of the pooled studies comparing pregnant hyperthyroid women who shifted between PTU and MMI with pregnant hyperthyroid women who did not receive any ATD treatment according to the risk of congenital anomalies.

(0.02MB).

The effect of antithyroid drugs on congenital malformations

As shown in Figure 5, five studies reported on congenital malformations after exposure to PTU or MMI. A meta-analysis of these five studies resulted in a pooled OR of 0.73, with a 95% CI of 0.56–0.96, indicating that PTU was a safer choice with respect to the risk of birth defects among pregnant women with hyperthyroidism.

Figure 5.

Forest plot of the odds ratios and 95% confidence intervals of the pooled studies comparing PTU-treated pregnant hyperthyroid women with MMI-treated pregnant hyperthyroid women according to the risk of congenital anomalies.

(0.03MB).

Several studies have linked hyperthyroidism during pregnancy with an increased risk of congenital anomalies. However, the evidence regarding the impact of ATDs such as PTU and MMI on pregnancy outcomes remains controversial. The preferred ATD during pregnancy in the USA is PTU, whereas in Europe, it is MMI 21,22.

In this study, we compared the risk of congenital anomalies among pregnant women with hyperthyroidism classified into three groups: those receiving PTU treatment, those receiving MMI treatment, and those receiving either PTU or MMI first and then shifting to MMI or PTU, respectively. In addition, we enrolled two control groups in this study: completely healthy pregnant women and women with hyperthyroidism who were not exposed to any ATD. Severe hyperthyroidism during pregnancy typically causes various complications for both the mother and the fetus 23. Thus, the pregnant women who were not exposed to any ATD either exhibited euthyroidism throughout pregnancy or exhibited hyperthyroidism that was observed late in pregnancy. The latter group of patients delivered before therapy.

Compared with hyperthyroid women not receiving an ATD or healthy pregnant controls, a significant increase in the rate of major anomalies was observed in those receiving MMI treatment. There was only a slight trend towards an increased risk of congenital malformations in infants whose mothers were treated with PTU compared with those whose mothers were healthy controls. The risk of birth defects for hyperthyroid women treated with PTU and those not receiving any ATD was similar. As the non-exposed group of women was largely healthy, the similar rates between the two aforementioned groups indicated that PTU was the preferred option according to the risk of congenital anomalies. However, one limitation to these studies was the confounding between the effect of hyperthyroidism itself and the effect of the drug in producing adverse fetal outcomes. It is reasonable to expect that the more severe examples of hyperthyroidism would be observed in the very women for whom drug treatment was prescribed, particularly at higher doses. Thus, the adverse fetal outcomes could have resulted from either the underlying severe hyperthyroidism or the treatment. To control for this confounding factor, we considered the eligible subjects for this study to be pregnant women with hyperthyroidism who received ATD treatment. Then, we compared PTU use with MMI use in relation to the overall rate of anomalies. Our data also supported the use of PTU. Taken together, these results indicated that PTU is a safer choice for the treatment of pregnant women with hyperthyroidism according to the risk of birth defects. This conclusion is in accordance with an American Thyroid Association statement supporting the use of PTU as the first-line agent for the management of hyperthyroidism during pregnancy 24.

A recent systematic review conducted by Hackmon et al. also described the safety of MMI and PTU during pregnancy 25. These authors concluded that MMI is a teratogen, which is consistent with our findings. In most cases associated with MMI embryopathy included in the case reports reviewed by Hackmon et al., exposure to MMI indeed occurred in the first trimester during the critical embryogenic period. In the present study, among the 6 studies examining the relationship of MMI exposure to the risk of birth defects, a total of 3 studies (Anderson et al., Yoshihara et al., and Momotani et al.) reported on the risk of congenital anomalies following intrauterine exposure in the first trimester. The findings of these studies showed that MMI treatment significantly increased the risk of congenital malformations. The remaining studies (Chen et al., Korelitz et al., and Wing et al), which did not describe whether ATD treatment was administered in the first trimester, failed to confirm a causal relationship between MMI and congenital malformations. This result was probably due to exposure after the period of organogenesis.

Shifts between PTU and MMI are not common in the treatment of patients with hyperthyroidism. Two of the included articles did not explain the reason that the doctors preferred to change the treatment, although this preference was likely related to potential concerns about the teratogenic effects of MMI in the first trimester and the hepatotoxicity of PTU during pregnancy 26,27. Thus, it was suggested that in pregnant women, PTU use should be restricted to the first trimester, and MMI should then be used during the remainder of pregnancy to minimize potential risks to the fetus and the mother. Our study illustrated that shifts between MMI and PTU may confer little protection against birth defects. This conclusion is inconsistent with the previous study conducted by Hackmon et al., who demonstrated that PTU should be administered during the first trimester, followed by a switch to MMI for the remainder of the pregnancy. One possible explanation for this disagreement might be as follows: due to severe PTU-induced hepatotoxicity, women with hyperthyroidism might be treated with MMI, and the shift from MMI to PTU may only occur when they find out that they are pregnant. Thus, there is a high probability that exposure to MMI occurs during the critical embryogenic period (4 to 10 weeks) because under most circumstances, women are actually pregnant for more than one month before they find out that they are pregnant. For instance, one study included in our meta-analysis reported that the mean time from the beginning of pregnancy to the shift to PTU treatment was 44 days. In addition, considering shifts between PTU and MMI, there were two types of drug prescription patterns observed in the included studies: from PTU to MMI and from MMI to PTU. Therefore, we should examine whether the prevalence of birth defects differs according to type of ATD prescription pattern.

However, there is no evidence from current trials to guide the choice between PTU followed by a switch to MMI and vice versa. Thus, it is certain that changes in ATD prescription patterns are not necessary during pregnancy. To avoid shifts in ATD use, it is recommended that women of child-bearing age choose PTU treatment before pregnancy to minimize the potential risk of congenital malformations.

Our research provides important population-based estimates of medication use that are relevant to the care of pregnant women with hyperthyroidism. However, a definitive answer to this question remains unclear because there are no available RCTs comparing antithyroid treatments in pregnant women with hyperthyroidism. Additional human epidemiology studies are needed, and new evidence-based recommendations should be developed for the treatment of women with hyperthyroidism during pregnancy.

Despite the lack of RCTs, we believe that our study provides potentially useful data to physicians prescribing ATDs to pregnant women with hyperthyroidism. The limited available evidence shows that PTU is a safer choice for treating pregnant women with hyperthyroidism according to the risk of birth defects but that shifting between MMI and PTU fails to provide protection against birth defects.

Li X conceived and designed the experiments. Liu GY supervised the data collection. Ma JL and Zhou L independently screened the articles.