Abstract:Abstract.Purpose behind developing these guidelines: Over one decade ago, the “Guidelines for the
Treatment of Graves’ Disease with Antithyroid Drug, 2006” (Japan Thyroid Association
(JTA)) were published as the standard drug therapy protocol for Graves’ disease. The
“Guidelines for the Treatment of Childhood-Onset Graves’ Disease with Antithyroid Drug in
Japan, 2008” were published to provide guidance on the treatment of pediatric patients.
Based on new evidence, a revised version of the “Guidelines for the T… Show more
“…The criteria for ATD discontinuation were normal thyroid function with a maintenance dose of MMI (≤5 mg/day) or CBZ (≤10 mg/day) for more than 6 months . The terms used in this study were defined as follows: Good initial response to ATD —time from diagnosis to keeping maintenance dose within six months. Remission —normal FT4, T3, and TSH levels without symptoms of hyperthyroidism for more than one year after ATD discontinuation. Relapse —high serum FT4 and T3 levels with low TSH levels after ATD discontinuation. A decrease in TRAb levels during the first year or the second year —TRAb levels at the end of the first year or the second year less than 50% of the levels at diagnosis. An increase in TRAb levels during the second year —TRAb levels at the end of the second year more than 50% greater than the levels at the end of the first year.Commercial kits were used to measure hormone levels and the TBII index.…”
Graves' disease is uncommon in children. The remission rate after antithyroid drugs (ATD) therapy is lower than in adults. We evaluated the clinical course of ATD therapy in children with Graves' disease in southern Taiwan to determine whether their biochemical markers could be used to predict remission in these patients. We retrospectively reviewed the clinical data of 53 children diagnosed with Graves' disease between 2009 and 2019. Clinical and biochemical parameters were analyzed for predictors of remission. About three‐fourths of the patients were female. Their median age at diagnosis was 13 years. No sex differences were found in most clinical characteristics. There was no correlation between thyroid‐stimulating hormone receptor antibody (TRAb) levels at diagnosis and thyroid function or adverse reactions to ATD. Relapse occurred in 62% of patients after discontinuation of first‐course ATD therapy. Three variables—good initial response to ATD, a decrease in TRAb levels during the first year after diagnosis, and a decrease in TRAb levels during the second year after diagnosis—were significant predictors of remission for more than 18 months. In conclusion, children with Graves' disease who had early ATD‐controlled Graves' disease and decreased TRAb levels during the first 2 years are likely to enter remission for more than 18 months.
“…The criteria for ATD discontinuation were normal thyroid function with a maintenance dose of MMI (≤5 mg/day) or CBZ (≤10 mg/day) for more than 6 months . The terms used in this study were defined as follows: Good initial response to ATD —time from diagnosis to keeping maintenance dose within six months. Remission —normal FT4, T3, and TSH levels without symptoms of hyperthyroidism for more than one year after ATD discontinuation. Relapse —high serum FT4 and T3 levels with low TSH levels after ATD discontinuation. A decrease in TRAb levels during the first year or the second year —TRAb levels at the end of the first year or the second year less than 50% of the levels at diagnosis. An increase in TRAb levels during the second year —TRAb levels at the end of the second year more than 50% greater than the levels at the end of the first year.Commercial kits were used to measure hormone levels and the TBII index.…”
Graves' disease is uncommon in children. The remission rate after antithyroid drugs (ATD) therapy is lower than in adults. We evaluated the clinical course of ATD therapy in children with Graves' disease in southern Taiwan to determine whether their biochemical markers could be used to predict remission in these patients. We retrospectively reviewed the clinical data of 53 children diagnosed with Graves' disease between 2009 and 2019. Clinical and biochemical parameters were analyzed for predictors of remission. About three‐fourths of the patients were female. Their median age at diagnosis was 13 years. No sex differences were found in most clinical characteristics. There was no correlation between thyroid‐stimulating hormone receptor antibody (TRAb) levels at diagnosis and thyroid function or adverse reactions to ATD. Relapse occurred in 62% of patients after discontinuation of first‐course ATD therapy. Three variables—good initial response to ATD, a decrease in TRAb levels during the first year after diagnosis, and a decrease in TRAb levels during the second year after diagnosis—were significant predictors of remission for more than 18 months. In conclusion, children with Graves' disease who had early ATD‐controlled Graves' disease and decreased TRAb levels during the first 2 years are likely to enter remission for more than 18 months.
“…We reviewed the NICE “Important Safety Information” for carbimazole, and the advice pertaining to safe prescribing of ATDs within international guidelines . We then developed 27 questions that examined both adherence to published advice and the use and interpretation of related diagnostic tests, and compiled these into an online survey using “Google Forms” (Google Drive Office Suite, Alphabet inc, Mountain View, CA, USA).…”
Section: Methodsmentioning
confidence: 99%
“…Only CBZ and PTU are available in the UK. The United States Food and Drug Administration released a warning in 2010 regarding the increased risk of hepatotoxicity associated with PTU in children and, as a result, CBZ is recommended as first‐line treatment, with the exception of the first trimester of pregnancy . ETA (European Thyroid Association) and ATA (American Thyroid Association) guidelines advise on treatment for adults and children.…”
Section: Introductionmentioning
confidence: 99%
“…The ATA recommends a treatment duration of 12‐24 months, and the ETA a treatment duration of 36 months prior to stopping ATD therapy in children to check for remission . JTA (Japanese Thyroid Association) guidelines are paediatric‐specific and recommend treatment with methimazole for a duration of 18‐24 months …”
Section: Introductionmentioning
confidence: 99%
“…ETA guidelines do not advocate one treatment regimen over the other but the ATA recommends DT. JTA guidelines recommend avoiding BR, citing the 2010 Cochrane Collaboration review that identified an increased risk of adverse reactions with this treatment strategy when compared to DT . However, it has been highlighted that some of the studies included in the Cochrane review, and in the BR section of the analyses, used an ATD dose that was much higher than routinely used in clinical practice .…”
Objective
We aimed to document current practice in the medical management of paediatric hyperthyroidism in the UK and compare to international recommendations.
Design
A 27‐question online survey distributed via an electronic newsletter in August 2018.
Participants
Responses from 48 members (11%) of the British Society for Paediatric Endocrinology and Diabetes.
Measurements
Information about antithyroid drug (ATD) preference, treatment duration, monitoring of full blood count (FBC), management of neutropaenia, agranulocytosis screening and patient education.
Results
Carbimazole is favoured by 98% of respondents and a “dose titration” regimen preferred over “block and replace” (65% vs 29%). TRAbs (thyroid‐stimulating hormone receptor antibodies) are used for diagnostic purposes by 85% and by 33% to look for evidence of disease remission. The majority (81%) treat for a minimum of 2 years before considering a trial off ATD. All respondents reported that they “always/usually” warn their patients about the risk of agranulocytosis before starting ATD, but written information is “rarely/never” provided by 63%. Sore throat (98%) and fever (92%) are the most commonly cited symptoms used to alert a patient to possible agranulocytosis. FBC is measured prior to treatment by 65% and measured periodically during treatment by 70%.
Conclusions
The management of paediatric hyperthyroidism with ATDs in the UK is not consistent with all international recommendations because a block and replace ATD regimen remains widely used. TRAbs are utilized at presentation, but underused for detecting disease remission. National consensus guidelines and written patient information may refine the management of paediatric patients on ATDs.
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