Different Outcomes of Neonatal Thyroid Function after Graves' Disease in Pregnancy: Patient Reports and Literature Review

IntroductionAn Israeli national survey found that 85% of pregnant women had urinary iodine content (UIC) levels below the adequacy range (<150 µg/L). Widespread desalinated water usage and no national fortification plan are possible causes. Studies assessing relationships between iodine status and maternal and neonatal thyroid function provided varying results. Our aims were to determine whether iodine deficiency was associated with altered maternal or neonatal thyroid function and the factors leading to iodine deficiency.MethodsA cross-sectional study including 100 healthy women without prior thyroid disease, in their first trimester of a singleton pregnancy were recruited from an HMO clinic in central Israel. The women were followed from their first trimester. All women completed a 24-h dietary recall and life habits questionnaires. We tested for UIC, maternal and neonatal thyroid function, maternal autoantibodies, and neonatal outcomes.ResultsMedian UIC in our cohort was 49 µg/L [25%–75% interquartile range (IQR) 16-91.5 µg/L], with 84% below adequacy range. No correlation was found between iodine deficiency and maternal or neonatal thyroid function which remained within normal ranges. Antibody status did not differ, but thyroglobulin levels were significantly higher in iodine insufficient subjects. UIC was higher in women consuming an iodine containing supplement. There was no association between UIC and dietary iodine content or water source.ConclusionsModerate iodine deficiency is common in our healthy pregnant women population. Our data imply that moderate iodine deficiency in pregnancy seem sufficient to maintain normal maternal and neonatal thyroid function.

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Therapeutic plasma exchange for Graves’ disease in pregnancy

Obstetric Medicine ◽

10.1177/1753495x211031328 ◽

2021 ◽

pp. 1753495X2110313

Author(s):

Matthew Lumchee ◽

Mimi Yue ◽

Josephine Laurie ◽

Adam Morton

Keyword(s):

Plasma Exchange ◽

Thyroid Function ◽

Therapeutic Plasma Exchange ◽

Graves Disease ◽

Close Monitoring ◽

Optimal Management ◽

Rapid Control ◽

Preconception Counselling ◽

Definitive Management ◽

In Pregnancy

Graves’ disease in pregnancy may be associated with maternal, fetal and neonatal complications, which are proportionate to the severity of hyperthyroidism. Optimal management is detailed preconception counselling, achievement of an euthyroid state prior to conception, and close monitoring of thyroid function and thyroid-stimulating antibodies together with judicious use of anti-thyroid medications during pregnancy. A case of Graves’ disease in pregnancy, complicated by pancytopenia, with a deterioration in thyroid function following cessation of thionamide therapy is described here. Therapeutic plasma exchange was subsequently used to achieve rapid control prior to thyroidectomy. Therapeutic plasma exchange is an effective treatment for hyperthyroidism where thionamides are ineffective or contraindicated, as a bridge to definitive management.

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ENDOCRINOLOGY IN PREGNANCY: Pregnancy and the incidence, diagnosing and therapy of Graves’ disease

Acta Endocrinologica ◽

10.1530/eje-16-0410 ◽

2016 ◽

Vol 175 (5) ◽

pp. R219-R230 ◽

Cited By ~ 14

Author(s):

Peter Laurberg ◽

Stine Linding Andersen

Keyword(s):

Thyroid Function ◽

Birth Defects ◽

Early Pregnancy ◽

Graves Disease ◽

Thyroid Function Tests ◽

Developmental Factors ◽

Normal Thyroid Function ◽

Important Concern ◽

And Control ◽

In Pregnancy

Thyroid hormones are essential developmental factors, and Graves’ disease (GD) may severely complicate a pregnancy. This review describes how pregnancy changes the risk of developing GD, how early pregnancy by several mechanisms leads to considerable changes in the results of the thyroid function tests used to diagnose hyperthyroidism, and how these changes may complicate the diagnosing of GD. Standard therapy of GD in pregnancy is anti-thyroid drugs. However, new studies have shown considerable risk of birth defects if these drugs are used in specific weeks of early pregnancy, and this should be taken into consideration when planning therapy and control of women who may in the future become pregnant. Early pregnancy is a period of major focus in GD, where pregnancy should be diagnosed as soon as possible, and where important and instant change in therapy may be warranted. Such change may be an immediate stop of anti-thyroid drug therapy in patients with a low risk of rapid relapse of hyperthyroidism, or it may be an immediate shift from methimazole/carbimazole (with risk of severe birth defects) to propylthiouracil (with less risk), or maybe to other types of therapy where no risk of birth defects have been observed. In the second half of pregnancy, an important concern is that not only the mother with GD but also her foetus should have normal thyroid function.

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Neonatal Thyroid Function after Propylthiouracil Therapy for Maternal Graves' Disease

New England Journal of Medicine ◽

10.1056/nejm198102263040907 ◽

1981 ◽

Vol 304 (9) ◽

pp. 525-528 ◽

Cited By ~ 114

Author(s):

Robert G. Cheron ◽

Michael M. Kaplan ◽

P. Reed Larsen ◽

Herbert A. Selenkow ◽

John F. Crigler

Keyword(s):

Thyroid Function ◽

Graves Disease ◽

Neonatal Thyroid Function

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Management of Graves' hyperthyroidism in pregnancy: focus on both maternal and foetal thyroid function, and caution against surgical thyroidectomy in pregnancy

Acta Endocrinologica ◽

10.1530/eje-08-0663 ◽

2009 ◽

Vol 160 (1) ◽

pp. 1-8 ◽

Cited By ~ 92

Author(s):

Peter Laurberg ◽

Claire Bournaud ◽

Jesper Karmisholt ◽

Jacques Orgiazzi

Keyword(s):

Drug Therapy ◽

Thyroid Function ◽

Antithyroid Drug ◽

Autoimmune Disorder ◽

Antithyroid Drugs ◽

Graves Disease ◽

Limited Effect ◽

Antithyroid Drug Therapy ◽

Maternal Thyroid ◽

In Pregnancy

Graves' disease is a common autoimmune disorder in women in fertile ages. The hyperthyroidism is causedby generation of TSH-receptor activating antibodies. In pregnancy both the antibodies and the antithyroid medication given to the mother pass the placenta and affect the foetal thyroid gland. Thyroid function should be controlled not only in the mother with Graves' hyperthyroidism but also in her foetus.The review includes two cases illustrating some of the problems in managing Graves' disease in pregnancy.Major threats to optimal foetal thyroid function are inadequate or over aggressive antithyroid drug therapy of the mother. It should be taken into account that antithyroid drugs tend to block the foetal thyroid function more effectively than the maternal thyroid function, and that levothyroxin (l-T4) given to the mother will have only a limited effect in the foetus.Surgical thyroidectomy of patients with Graves' hyperthyroidism does not lead to immediate remission of the autoimmune abnormality, and the combination thyroidectomy+withdrawal of antithyroid medication+l-T4 replacement of the mother involves a high risk of foetal hyperthyroidism.ConclusionAntithyroid drug therapy of pregnant women with Graves' hyperthyroidism should be balanced to control both maternal and foetal thyroid function. Surgical thyroidectomy of a pregnant woman with active disease may lead to isolated foetal hyperthyroidism.

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Abstract #1202: A Case of Graves’ Disease With Fluctuating Thyroid Function

Endocrine Practice ◽

10.1016/s1530-891x(20)44852-9 ◽

2016 ◽

Vol 22 ◽

pp. 305-306

Author(s):

Sheela Metgud ◽

Anup Kumar ◽

Erin Drever ◽

Tahira Yasmeen

Keyword(s):

Thyroid Function ◽

Graves Disease

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Faculty Opinions recommendation of Maternal and perinatal outcomes in pregnancy-associated melanoma. Report of two cases and a systematic literature review.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.727651280.793574717 ◽

2020 ◽

Author(s):

Teresa Woodruff

Keyword(s):

Literature Review ◽

Systematic Literature Review ◽

Perinatal Outcomes ◽

In Pregnancy

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Graves' disease and radioiodine therapy

Nuklearmedizin ◽

10.3413/nukmed-0145 ◽

2008 ◽

Vol 47 (04) ◽

pp. 153-166 ◽

Cited By ~ 10

Author(s):

I. Weber ◽

W. Eschner ◽

F. Sudbrock ◽

M. Schmidt ◽

M. Dietlein ◽

...

Keyword(s):

Success Rate ◽

Thyroid Function ◽

Therapeutic Dose ◽

Radioiodine Therapy ◽

Antithyroid Drugs ◽

Graves Disease ◽

Inclusion Criteria ◽

End Point ◽

Point Measure ◽

The Impact

SummaryAim: This study was performed to analyse the impact of the choice of antithyroid drugs (ATD) on the outcome of ablative radioiodine therapy (RIT) in patients with Graves' disease. Patients, material, methods: A total of 571 consecutive patients were observed for 12 months after RIT between July 2001 and June 2004. Inclusion criteria were the confirmed diagnosis of Graves' disease, compensation of hyperthyroidism and withdrawal of ATD two days before preliminary radioiodine-testing and RIT. The intended dose of 250 Gy was calculated from the results of the radioiodine test and the therapeutically achieved dose was measured by serial uptake measurements. The end-point measure was thyroid function 12 months after RIT; success was defined as elimination of hyperthyroidism. The pretreatment ATD was retrospectively correlated with the results achieved. Results: Relief from hyperthyroidism was achieved in 96 % of patients. 472 patients were treated with carbimazole or methimazole (CMI) and 61 with propylthiouracil (PTU). 38 patients had no thyrostatic drugs (ND) prior to RIT. The success rate was equal in all groups (CMI 451/472; PTU 61/61; ND 37/38; p=0.22). Conclusion: Thyrostatic treatment with PTU achieves excellent results in ablative RIT, using an accurate dosimetric approach with an achieved post-therapeutic dose of more than 200 Gy.

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