| Literature DB >> 23762777 |
Shahram Alamdari1, Fereidoun Azizi, Hossein Delshad, Farzaneh Sarvghadi, Atieh Amouzegar, Ladan Mehran.
Abstract
Appropriate diagnosis and treatment of hyperthyroidism during pregnancy are of outmost importance, because hyperthyroidism has major adverse impact on both mother and fetus. Since data on the management of thyroid dysfunction during pregnancy is rapidly evolving, two guidelines have been developed by the American Thyroid Association and the Endocrine society in the last 2 years. We compare here the recommendations of these two guidelines regarding management of hyperthyroidism during pregnancy. The comparison reveals no disagreement or controversy on the various aspects of diagnosis and treatment of hyperthyroidism during pregnancy between the two guidelines. Propylthiouracil has been considered as the first-line drug for treatment of hyperthyroidism in the first trimester of pregnancy. In the second trimester, consideration should be given to switching to methimazole for the rest of pregnancy. Methimazole is also the drug of choice in lactating hyperthyroid women.Entities:
Year: 2013 PMID: 23762777 PMCID: PMC3674680 DOI: 10.1155/2013/878467
Source DB: PubMed Journal: J Thyroid Res
Comparison of recommendations of American Thyroid Association and Endocrine Society on the management of hyperthyroidism before pregnancy and on the diagnosis of hyperthyroidism and pregnancy.
| Topic | Recommendations | |
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| American Thyroid Association (2011) | Endocrine Society (2012) | |
| Management before pregnancy | Same (R and T) | For overt hyperthyroidism due to Graves' disease or thyroid nodules, antithyroid drug (ATD) therapy should be either initiated (before pregnancy if possible, and for those with new diagnoses) or adjusted (for those with a prior history) to maintain the maternal thyroid hormone levels for free T4 at or just above the upper limit of the nonpregnant reference range, or to maintain total T4 at 1.5 times the upper limit of the normal reference range or the free T4 index in the upper limit of the normal reference range. |
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| Thyroid function | In the presence of a suppressed serum TSH in the first trimester (TSH < 0.1 mIU/L), a history and physical examination are indicated. FT4 measurements should be obtained in all patients. Measurement of TT3 and TRAb may be helpful in establishing a diagnosis of hyperthyroidism. | Same (R) |
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| Ultrasonography | There is not enough evidence to recommend for or against the use of thyroid ultrasound in differentiating the cause of hyperthyroidism in pregnancy. | None |
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| Scanning and | Radioactive iodine (RAI) scanning or radioiodine uptake determination should not be performed in pregnancy. | None |
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| Differentiation of | Same (T) | Differentiation of Graves' from gestational thyrotoxicosis is supported by the presence of clinical evidence of autoimmunity, typical goiter, and presence of TSH receptor antibodies (TRAb). TPO-Ab may be present in either case. |
Comparison of recommendations of American Thyroid Association and Endocrine Society on the treatment of hyperthyroidism in pregnancy.
| Topic | Recommendations | |
|---|---|---|
| American Thyroid Association (2011) | Endocrine Society (2012) | |
| Antithyroid (ATD) treatment | PTU is preferred for the treatment of hyperthyroidism in the first trimester, and patients on MMI should be switched to PTU if pregnancy is confirmed in the first trimester. Following the first trimester, consideration should be given to switching to MMI. | Propylthiouracil (PTU), if available, is recommended as the first-line drug for treatment of hyperthyroidism during the first trimester of pregnancy because of the possible association of methimazole (MMI) with specific congenital abnormalities that occur during first trimester organogenesis, and MMI may also be prescribed if PTU is not available or if a patient cannot tolerate or has an adverse response to PTU. |
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| Combination of LT4 and ATD | A combination regimen of T4 and an ATD should not be used in pregnancy, except in the rare situation of fetal hyperthyroidism. | None |
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| Monitoring liver function in women on PTU | None | Although liver toxicity may appear abruptly, it is reasonable to monitor liver function in pregnant women on PTU every 3-4 weeks and to encourage patients to promptly report any new symptoms. |
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| Monitoring of thyroid function | In women being treated with ATDs in pregnancy, FT4 and TSH should be monitored approximately every 2–6 weeks. The primary goal is a serum FT4 at or moderately above the normal reference range. | Same (T) |
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| Surgery | Same (R and T) | Subtotal thyroidectomy may be indicated during pregnancy as therapy for maternal Graves' disease if (1) a patient has a severe adverse reaction to ATD therapy (2) persistently high doses of ATD are required (over 30 mg/d of MMI or 450 mg/d of PTU) or (3) a patient is nonadherent to ATD therapy and has uncontrolled hyperthyroidism. The optimal timing of surgery is in the second trimester. |
Comparison of recommendations of American Thyroid Association and Endocrine Society on the fetal aspects of hyperthyroidism in pregnancy.
| Topic | Recommendations | |
|---|---|---|
| American Thyroid Association (2011) | Endocrine Society (2012) | |
| Thyroid receptor antibodies (TRAb) | If the patient has a past or present history of Graves' disease, a maternal serum determination of TRAb should be obtained at 20–24 weeks gestation. | TRAb should be measured by 22-week gestational age in mothers with (1) current Graves' disease; or (2) a history of Graves' disease and treatment with 131I or thyroidectomy before pregnancy; (3) a previous neonate with Graves' disease; or (4) previously elevated TRAb |
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| Fetal Surveillance | Fetal surveillance with serial ultrasounds should be performed in women who have uncontrolled hyperthyroidism and/or women with high TRAb levels (greater than three times the upper limit of normal). A consultation with an experienced obstetrician or maternal-fetal medicine specialist is optimal. Such monitoring may include ultrasound for heart rate, growth, amniotic fluid volume, and fetal goiter. | In women with TRAb or thyroid-stimulating Ig elevated at least 2- to 3-fold the normal level and in women treated with ATD, maternal free T4, and fetal thyroid dysfunction should be screened for during the fetal anatomy ultrasound done in the 18th–22nd week and repeated every 4–6 weeks or as clinically indicated. Evidence of fetal thyroid dysfunction could include thyroid enlargement, growth restriction, hydrops, presence of goiter, advanced bone age, tachycardia, or cardiac failure, if fetal hyperthyroidism is diagnosed and thought to endanger the pregnancy, treatment using MMI or PTU should be given with frequent clinical, laboratory, and ultrasound monitoring. |
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| Umbilical blood sampling | Cordocentesis should be used in extremely rare circumstances and performed in an appropriate setting. It may occasionally be of use when fetal goiter is detected in women taking ATDs to help determine whether the fetus is hyperthyroid or hypothyroid. | Same (R) |
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| Evaluation of newborn | Same (T) | All newborns of mothers with Graves' disease (except those with negative TRAb and not requiring ATD) should be evaluated by a medical care provider for thyroid dysfunction and treated if necessary. |
Comparison of recommendations of American Thyroid Association and Endocrine Society on other aspects of hyperthyroidism in pregnancy.
| Topic | Recommendations | |
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| American Thyroid Association (2011) | Endocrine Society (2012) | |
| Management of | The appropriate management of women with gestational hyperthyroidism and hyperemesis gravidarum includes supportive therapy, management of dehydration, and hospitalization if needed. | Most women with hyperemesis gravidarum, clinical hyperthyroidism, suppressed TSH, and elevated free T4 do not require ATD treatment. Clinical judgment should be followed in women who appear significantly thyrotoxic or who have in addition serum total T3 values above the reference range for pregnancy. Beta blockers such as metoprolol may be helpful and may be used with obstetrical agreement. |
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| Subclinical hypothyroidism | Same (T) | There is no evidence that treatment of subclinical hyperthyroidism improves pregnancy outcome, and treatment could potentially adversely affect fetal outcome. |