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The Time Is Not Ripe To Screen

Division of Endocrinology Stanford University School of Medicine and Santa Clara Valley Medical Center San Jose, California 95128

	Introduction

Top Introduction Screening for thyroid disease... Screening for postpartum... Conclusion References

 
AT FIRST GLANCE, screening for postpartum thyroiditis (PPT) appears to be an attractive and possibly even a cost-effective strategy. The disorder is quite common, affecting in the range of 4–6% of all postpartum women (1). In the United States, where there are approximately 4 million live births annually (2), this means that PPT afflicts nearly 200,000 women each year. The symptoms associated with PPT are often subtle and difficult to distinguish from symptoms frequently present during the postpartum period. Those women at high risk for PPT are easy to identify because PPT is an autoimmune disease in which most patients have elevated serum levels of thyroid autoantibodies. It is generally assumed that over 20% of women with PPT will eventually develop permanent hypothyroidism within a 5-yr period (3, 4). Finally, PPT is easy to treat when symptoms are present by employing beta-blockers for the hyperthyroid phase and levothyroxine for the hypothyroid phase of the disorder (5).

On closer scrutiny, however, the screening strategy loses some of its initial appeal. Although PPT is common, symptoms during the hyperthyroid and hypothyroid phases of the illness are often mild in degree and brief in duration and, consequently, may not require treatment. When symptoms are moderate or severe in degree they should be recognized clinically, although this will require more education of primary care physicians and postpartum patients about PPT. Which thyroid autoantibody assay should be used for screening and when the assay should be performed have not been completely resolved. Furthermore, there is a lack of knowledge about how to follow patients with a positive antibody assay. Should a serum TSH level be done only when they are symptomatic, or should serial TSH levels be done and, if so, at what intervals? Finally and most importantly, there has been no prospective diagnostic and therapeutic trial to date that tells us whether or not a screening program would be beneficial.

We will initially discuss screening for thyroid disease in general to set the stage for a detailed discussion of screening for PPT. Available data and studies on these important issues will lead to the conclusion that the time is not yet ripe to recommend a screening program for all pregnant or postpartum women to identify those who are at risk for or who have PPT.

	Screening for thyroid disease in general

Top Introduction Screening for thyroid disease... Screening for postpartum... Conclusion References

 
In general, screening may be defined as testing for the presence of a disease or the risk of a disease when no known signs or symptoms of the disease are present, with the purpose of improving health outcomes in the target population (6). Screening recommendations for thyroid disease involve an assessment of age, gender, family history, and associated physiologic or pathophysiologic conditions. In addition to specifying who should be screened, such recommendations also need to specify which tests should be employed, how frequently they should be employed, and where they should be employed.

Presently, there is only one universally agreed-upon strategy in screening for thyroid disease, which is that neonates should be screened for congenital hypothyroidism with a blood TSH or total T4 assay shortly after birth in the hospital. In 1990, the American Thyroid Association (ATA) recommended against screening for thyroid disease in asymptomatic subjects in the general population who were not at high risk for thyroid disease and its consequences (7). The Canadian Task Force on the Periodic Health Examination in 1994 (8), and the United States Preventative Services Task Force (USPSTF) in 1996 (9), concurred in this recommendation against general screening. All agencies recommend screening for hypothyroidism in neonates even though it is infrequent (1 case per 4,000 births). The ATA recommends screening with tests of thyroid function in certain higher risk situations, such as in elderly patients, those with a family history of thyroid disease, individuals with autoimmune diseases such as type I diabetes mellitus, and in postpartum women at 4–8 weeks (7). The USPSTF adds the high risk group of persons with Down’s syndrome, and notes that at the present time there is insufficient evidence to recommend for or against screening for thyroid disease in any of the childhood or adult high risk groups, including postpartum women (9). They do recommend that clinicians should remain alert for subtle signs and symptoms of thyroid dysfunction and keep a low threshold for evaluating thyroid status in such high risk subjects.

Recently, one study has demonstrated by cost-utility decision analysis that it is cost-effective to screen for mild thyroid failure with a serum TSH assay at 5-yr intervals starting at age 35 yr for both men and women, and that such screening is especially recommended for elderly women (10). More recently, the American College of Physicians has recommended screening for unsuspected but symptomatic hypothyroidism and hyperthyroidism in women over 50 yr of age, employing a sensitive serum TSH assay (11, 12). They further note that there is insufficient evidence at present to recommend for or against screening for subclinical hypothyroidism or subclinical hyperthyroidism, although this latter recommendation has been criticized (13).

Thus, from the general literature on screening for thyroid disease, there is little to help guide us in a decision about screening for PPT, and what there is remains controversial. In the presence of conflicting recommendations from prestigious national agencies, and in the absence of published cost-benefit analyses or prospective controlled clinical trials, we are compelled to form a conclusion about the merits of screening for PPT on other grounds, employing available studies on the epidemiologic, laboratory, and clinical characteristics of PPT.

	Screening for postpartum thyroiditis

Top Introduction Screening for thyroid disease... Screening for postpartum... Conclusion References

 
In order to develop a strategy of screening for PPT it is necessary to review the epidemiology of the disorder and assess its varied clinical manifestations so we can answer the questions of what are we screening for, what tests should we use for screening, when we should screen, and whether or not screening is superior to clinical ascertainment of PPT.

PPT is an autoimmune disorder characterized by a destructive lymphocytic infiltration of the thyroid gland, very often with accompanying circulating thyroid autoantibodies, which can manifest itself as transient hyperthyroidism, transient hypothyroidism, or permanent hypothyroidism. These manifestations result from activation of immunological changes that occur in the first postpartum year. The symptoms of PPT are those of hyperthyroidism or hypothyroidism added to a background of symptoms commonly found in the postpartum period, such as fatigue, tiredness, depression, emotional lability, and anxiety. These symptoms can be mild or severe and transient or prolonged. Thus, PPT is a protean disorder with varied presentations at varied times hiding in the shadow of common postpartum symptoms, which renders the development of a screening strategy very difficult. The epidemiology of PPT is presented in Table 1,where the outcome of 1,000 hypothetical unselected postpartum women is traced, assuming that 5% of the women will develop PPT, 10% of the women will be positive for serum thyroid peroxidase autoantibodies (TPO-Ab), nearly 50% of the women with a positive TPO-Ab titer will develop PPT, and that 90% of women with PPT will have a positive TPO-Ab titer. The data in this table have been derived from several reviews of numerous studies on the incidence of PPT and the prevalence of positive TPO-Ab titers in postpartum women (1, 14). The incidence of PPT in these studies varies by over an order of magnitude from 1.1% to 16.7%, which may be explained in part by variations in geographical location, definition of PPT, duration of studies, and frequency of testing. A critical evaluation of many of the studies suggests that the incidence of symptomatic PPT is about 5% (1). The incidence data on permanent overt hypothyroidism in Table 1 and Table 2 hasbeen derived from 5 separate studies in which patients with PPT have been followed for 3–5 yr (3, 4, 15, 16, 17).

If a screening program for PPT is employed, what tests should be used and when should they be done? If all postpartum women were screened with a sensitive TSH assay at 2- to 3-month intervals, then nearly all cases of PPT would be detected. However, this strategy is clearly impractical and too costly. In the United States, where there are 4 million live births per year, this would entail approximately 12 million TSH assays at a cost of about 250 million dollars per year. A more reasonable strategy would be to screen all postpartum women with a sensitive thyroid autoantibody assay, such as TPO-Ab, and then follow the women testing positive with several TSH assays during the 1-yr postpartum period. From the data in Table 1, this would entail 4 million TPO-Ab assays and about 1.2 million TSH assays per year at a cost of about 100 million dollars per year to detect 200,000 cases of PPT at a cost of $500 per case detected, many of which would be mild and would not need treatment. A clinical approach to detection of PPT would cost 30–50 million dollars per year, assuming that 30–50% of 4 million postpartum women were symptomatic and tested with a single TSH assay, and that all postpartum women received a $2 pamphlet alerting them to the symptoms of PPT. It is possible that benefits from a program employing clinical astuteness would be comparable to a screening program. However, an accurate cost-benefit is not possible until good studies are available detailing the clinical presentation of PPT and how they respond to therapy. Unfortunately, no study has yet been published to demonstrate that such a screening strategy would be superior in cost or in benefit to thorough clinical assessment of postpartum women. Although the sensitivity of the TPO-Ab assay in identifying women who will develop PPT is generally about 90%, the range in a number of studies is from 50–100% (14). In a recent, thorough study from The Netherlands the sensitivity was 67%. This means that screening with a TPO-Ab assay would miss 33% of the women who develop PPT and, thus, casts doubt on the recommendation of this strategy for all countries (24, 25). Certain women with a known high risk for PPT, such as those with type I diabetes mellitus, previous autoimmune thyroid disease (AITD), or a strong family history of AITD should be followed closely under any circumstances by thorough clinical and, if necessary, biochemical scrutiny (26, 27, 28).

Even if screening for PPT is not superior to careful clinical assessment in the diagnosis and treatment of symptomatic transient hyperthyroidism or hypothyroidism, should screening be employed to identify postpartum women who are at risk for permanent overt hypothyroidism? The long-term sequelae of PPT have been recently reviewed (29), and the results of those studies that have followed patients with PPT for 3 yr or longer are summarized in Table 2. Several important observations can be extracted from this table. First, the mean rate of progression from PPT to permanent overt hypothyroidism over a 5-yr period in the 5 studies is 3.6% per year. This is very close to the rate at which all adult women in the community with a positive TPO-Ab titer progress to spontaneous overt hypothyroidism as determined in the renowned Wickham survey, which observed rates of 4.3% per year when the serum TSH level was elevated, and 2.1% per year when the TSH level was normal (30). Second, the mean rate of progression of all postpartum women to permanent overt hypothyroidism over a 5-yr period in the 5 studies is 1.8 cases/1000 women/yr, very close to the rate at which all women develop spontaneous hypothyroidism (3.5 cases/1000 women/yr for all women, and 1.4 cases/1000 women/yr for young women in their child-bearing years) seen in the Wickham survey (30). Thus, the rate of progression to spontaneous permanent hypothyroidism in postpartum women with and without PPT is virtually the same as the rate seen in the Wickham survey in all young women with and without positive TPO-Ab titers.

	Conclusion

Top Introduction Screening for thyroid disease... Screening for postpartum... Conclusion References

 
The time is not yet ripe to recommend a screening program for all postpartum women to detect PPT, even though the disorder is common. The basic problem is that there is a lack of knowledge at present about how to screen, when to screen, and whether or not treatment makes a difference for those women with unrecognized mild or moderate thyroid dysfunction. Permanent hypothyroidism occurs at about the same rate of incidence in postpartum women as in all young women, and in both groups is confined almost exclusively to those with preexisting AITD. Whether or not young women, including postpartum women, should be screened to detect those who have or are at risk for permanent hypothyroidism remains an open question until further studies clarify the issue.

Finally, a recommendation against screening postpartum women for PPT at the present time should not be construed to mean that clinical vigilance is not warranted. In general, the thorough care that women receive during their pregnancy has no counterpart during their first postpartum year, as attention in the family and in the medical system shifts from the mother to the infant. Thus, there is a compelling need to educate postpartum women and the physicians who care for them about PPT and other important postpartum afflictions.

	References

Top Introduction Screening for thyroid disease... Screening for postpartum... Conclusion References

 

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