Effects of methimazole and propylthiouracil exposure during pregnancy on the risk of neonatal congenital malformations: A meta-analysis

Song, Rongjing; Lin, Hepu; Chen, Yue; Zhang, Xiuying

doi:10.1371/journal.pone.0180108

Cited by 39 publications

(38 citation statements)

References 30 publications

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“…Epidemiological studies presented mixed results of no increased risk of congenital anomalies with MMI/CMZ exposure in some studies (Andersen et al, 2017;Chen et al, 2011;Di Gianantonio et al, 2001;Gianetti et al, 2015;Korelitz et al, 2013;Lo et al, 2015; compared to increased risk in other studies (Andersen et al, 2013;Seo et al, 2018;Yoshihara et al, 2012). Metaanalyses have demonstrated increased risks of anomalies with exposure to MMI/CMZ (Li, Liu, Ma, & Zhou, 2015;Li, Zheng, et al, 2015;Song, Lin, Chen, Zhang, & Feng, 2017).…”

Section: And Carbinazolementioning

confidence: 99%

Teratogen update: Antithyroid medications

Romeo

Običan

2020

Birth Defects Research

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Objective Thyroid disorders including hyperthyroidism are common during pregnancy. Untreated hyperthyroidism can result in adverse outcomes for pregnancy. Methods Iodine, propylthiouracil (PTU), carbimazole (CMZ), and methimazole (MMI) are common medications for hyperthyroidism treatment. The literature regarding antithyroid medication use in pregnancy and breastfeeding is reviewed. Results Animal studies for PTU have suggested congenital anomalies while animal studies for MMI have only indicated adverse outcomes at higher doses than used in humans. Epidemiological studies have noted an increased risk of congenital anomalies for PTU less often than CMZ or MMI but the epidemiological evidence remains mixed. A pattern of anomalies has been described for CMZ and MMI, from both case and epidemiological studies, including choanal atresia, aplasia cutis congenita, and other facial, heart, gastrointestinal, and skin anomalies. Closer examination of cases indicates that a few cases of the anomalies have occurred without exposure to CMZ or MMI and outside of the proposed critical period. PTU has a small risk of hepatotoxicity which rarely results in liver transplantation and death. Some authors have suggested that PTU be prescribed in early pregnancy and switched to MMI in late pregnancy. Untreated hyperthyroidism, from either a lack of medications or switching medications during the first trimester, may also increase the chance of congenital anomalies. Multiple case studies and larger epidemiological studies have failed to provide clear, consistent outcomes for the use of PTU, CMZ, and MMI in pregnancy. MMI and PTU both enter the breastmilk in small amounts. Conclusion Additional research is needed to assist in the medical management and exposure counseling of pregnant and breastfeeding women with hyperthyroidism.

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Section: And Carbinazolementioning

confidence: 99%

Teratogen update: Antithyroid medications

Romeo

Običan

2020

Birth Defects Research

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“…For example, in a young woman who desires future pregnancy, RAI and surgery are favored because of the increased incidence of congenital malformations seen with ATDs during pregnancy. 31,56 However, ATDs are favored in patients with a high likelihood of remission or with severe GO. Thyroidectomy is preferred when there are symptoms of compression from large goiters, suspicious nodules, or moderate to severe and active orbitopathy in patients who cannot tolerate ATDs.…”

Section: Article Highlightsmentioning

confidence: 99%

“…However, if hyperthyroidism develops or persists during pregnancy, PTU is preferred during the first trimester because of the increased risk of serious birth defects associated with methimazole and carbimazole (odds ratio, 1.9 for methimazole/carbimazole vs PTU). 31 The risk for teratogenicity declines after week 10 of pregnancy, and thus PTU therapy is usually converted to methimazole because of the increased risk of hepatotoxicity from PTU. Given the risk of dysthyroidism associated with these therapeutic changes and the known teratogenicity of PTU itself, 58 these changes are still a matter of debate.…”

Section: Article Highlightsmentioning

confidence: 99%

Thyrotoxicosis: Diagnosis and Management

Sharma

Stan

2019

Mayo Clinic Proceedings

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Thyrotoxicosis is the clinical manifestation of excess thyroid hormone action at the tissue level due to inappropriately high circulating thyroid hormone concentrations. Hyperthyroidism, a subset of thyrotoxicosis, refers specifically to excess thyroid hormone synthesis and secretion by the thyroid gland. We performed a review of the literature on these topics utilizing published data in PubMed and MEDLINE. In this review, we discuss the more common etiologies of thyrotoxicosis, focusing on the current approach to diagnosis and management, new trends in those directions, and potential upcoming changes in the field.

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“…In the first quarter: Propylthiouracil can be used as low as possible during the first trimester of pregnancy [2,5]. In the 2nd and / or 3rd trimester, due to the undesirable liver effects of the PTU, it is preferable, if possible, to relieve the PTU with Carbimazole beyond the 1st trimester [4][5]14]. If PTU is maintained, use the lowest possible dosage.…”

Section: Treatmentmentioning

confidence: 99%

Hyperthyroid Fetal Goiter: A Case Report

Loue¹

2019

JGO

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The persistent presence of maternal thyroid-stimulating hormone receptor antibody in patients with Graves'disease could cause fetal hyperthyroid goiter during pregnancy. The recognition and treatment of hyperthyroid fetal goiter are believed to be very important to optimize growth and intellectual development in affected fetuses. We report here, a case of a hyperthyroid fetal goiter identified by ultrasound exam at 27 weeks 5 days of gestation in a women having Graves' disease and on antithyroid drugs therapy. This observation shows the fetal risk associated with the persistence of anti-TSH receptor antibodies in mothers with Graves' disease and the possibility of fetal approach.

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Effects of methimazole and propylthiouracil exposure during pregnancy on the risk of neonatal congenital malformations: A meta-analysis

Cited by 39 publications

References 30 publications

Teratogen update: Antithyroid medications

Teratogen update: Antithyroid medications

Thyrotoxicosis: Diagnosis and Management

Hyperthyroid Fetal Goiter: A Case Report

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