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Antithyroid agent

April 12, 2024

An antithyroid agent is a hormone inhibitor acting upon thyroid hormones.

The main antithyroid drugs are carbimazole (in the UK), methimazole (in the US), and propylthiouracil (PTU). A less common antithyroid agent is potassium perchlorate.

Classification based on mechanisms of action edit

The mechanisms of action of antithyroid drugs are not completely understood. Based on their mechanisms of action, the drugs are classified into following six classes.

Thyroid hormone synthesis inhbitors edit

These drugs probably inhibit the enzyme thyroid peroxidase (a.k.a. thyroperoxidase), decreasing iodide oxidation, iodination of tyrosyl residues in thyroglobulin, and coupling of iodotyrosyl and iodothyronyl residues.[1] It is thought that they inhibit the thyroperoxidase-catalyzed oxidation reactions by acting as substrates for the postulated peroxidase-iodine complex, thus competitively inhibiting the interaction with the amino acid tyrosine. The most common drugs in this class are thioamides, which include propylthiouracil, methimazole and its prodrug carbimazole.

Additionally, propylthiouracil may reduce the de-iodination of thyroxine (tetraiodothyronine; T4) into triiodothyronine (T3) in peripheral tissues.[2]

Lugol's iodine is used to temporarily block thyroid hormone synthesis before surgeries.[3] It is also used to treat patients with thyroid storm or, more commonly, to reduce thyroid vascularity before thyroidectomy (surgical removal of the thyroid gland).[4]

Iodide uptake inhibitors edit

They decrease uptake of iodide ions (I) into follicular cells of the thyroid gland. Since their molecules have structural similarities with the iodide ion, they compete with iodide for being transported by the sodium/iodide symporter, which is a transporter protein that co-transports Na+ and I ions. Iodide transport is a key step in the biosynthesis of the thyroid hormones T4 and T3.[5][6] For example, potassium perchlorate competitively inhibits the active iodide transport mechanism in the thyroid gland, which has the capacity to selectively concentrate iodide against a large concentration gradient.[5][6]

Besides perchlorates, other examples of iodide uptake inhibitors include pertechnetates, thiocyanates, nitrates.[7]

These drugs are no longer used due to high toxicity and adverse effects.[8][9]

Thyroid hormone release inhibitors edit

They inhibit release (secretion) of thyroid hormones by the thyroid gland. The most studied drug in this class is lithium, which inhibits thyroid hormone secretion by inhibiting iodotyrosine coupling, thyroidal iodide uptake, and alteration in structure of thyroglobulin,[10] a protein which acts as a substrate for the synthesis of thyroid hormones and storage of inactive forms of T3, T4 and iodine within the lumen of thyroid follicular cells.[11] Since lithium is neither metabolized nor protein-bound, its bioavailability usually is close to 100%.[12] Hence, there are risks of serious side effects such as lithium toxicity, hypothyroidism, and diabetes insipidus.[13]

Excess iodine edit

Excessive iodine intake can temporarily inhibit production of thyroid hormones. This occurs because of the Wolff-Chaikoff effect, which is a phenomenon of rejection of large quantities of iodine by the thyroid gland, therefore preventing it from synthesizing large quantities of thyroid hormones.[14]

Iodine radiopharmaceuticals edit

Main articles: Isotopes of iodine and radiopharmaceutical

They are radioisotopes of iodine. In small doses, when they are taken up by overactive thyroid follicular cells, they emit small amounts of beta radiation that destroys not all, but many thyroid follicular cells, thereby reducing thyroid hormone production.[15] This is a form of targeted therapy for hyperthyroidism. Since even low levels of ionizing radiation are highly mutagenic and can cause cancer,[16] less toxic iodine isotopes such as iodine-123[17] are more commonly used in nuclear imaging, while iodine-131 is used for its cytolytic (cell-destroying) effects in hyperthyroidism and thyroid tumors.[15]

Thyroid hormone receptor antagonists edit

Also called TR antagonists, they inhibit action of thyroid hormones by blocking TR receptors (thyroid hormone receptors). Antagonist 1-850 and its derivatives have been found to be coactivator interaction inhibitors, which interfere with the interaction between TR receptors and coactivator proteins such as nuclear hormone receptor coregulator (NRC). As a result, the receptors are unable to recruit coactivators, causing stoppage of transcription of target genes, thereby preventing activation of TR receptors, ultimately leading to inhibition of effects of thyroid hormones because they can bind to only inactive TR receptors, and these receptors can't be activated in presence of TR antagonists.[18] Antagonist 1-850 has also been found to inhibit binding of [125I]T3[a] to TRs in intact GH4 cells.[18]

Adverse effects edit

The most dangerous side effect is agranulocytosis (1/250, more in PTU); this is an idiosyncratic reaction which generally resolves on cessation of drug. It occurs in about 0.2 to 0.3% of cases treated with antithyroid drugs.[19] Other side effects include granulocytopenia (dose dependent, which improves on cessation of the drug) and aplastic anemia, and in case of propylthiouracil, severe, fulminant liver failure.[20] Patients on these medications should see a doctor if they develop sore throat or fever.

The most common side effects are rash and peripheral neuritis.[21] These drugs also cross the placenta and are secreted in breast milk.[22]

Graves' disease edit

In Graves' disease, treatment with antithyroid medications must be given for six months to two years, in order to be effective. Even then, upon cessation of the drugs, the hyperthyroid state may recur. Side effects of the antithyroid medications include a potentially fatal reduction in the level of white blood cells.

A randomized control trial testing single dose treatment for Graves' found methimazole achieved euthyroidism (normal thyroid function that occurs within normal serum levels of TSH and T4[23]) more effectively after 12 weeks than did propylthiouracil (77.1% on methimazole 15 mg vs 19.4% in the propylthiouracil 150 mg groups).[24] But generally both drugs are considered equivalent.

A study has shown no difference in outcome for adding thyroxine to antithyroid medication and continuing thyroxine versus placebo after antithyroid medication withdrawal. However, two markers were found that can help predict the risk of recurrence. These two markers are an elevated level of thyroid stimulating hormone receptor antibodies (TSHR-Ab) and smoking. A positive TSHR-Ab at the end of antithyroid drug treatment increases the risk of recurrence to 90% (sensitivity 39%, specificity 98%), a negative TSHR-Ab at the end of antithyroid drug treatment is associated with a 78% chance of remaining in remission. Smoking was shown to have an impact independent to a positive TSHR-Ab.[25]

Competitive antagonists of thyroid stimulating hormone receptors are currently being investigated as a possible treatment for Grave's disease.

See also edit

Notes edit

  1. ^ [125I]T3 is a radiopharmaceutical formulation of triiodothyronine having iodine-125 atoms instead of iodine.

References edit

  1. ^ . www.sciencedirect.com. Archived from the original on 2023-09-27. Retrieved 2023-10-03.
  2. ^ Manna D, Roy G, Mugesh G (2013). "Antithyroid Drugs and their Analogues: Synthesis, Structure and Mechanism of Action". Acc. Chem. Res. 46 (11): 2706–15. doi:10.1021/ar4001229. PMID 23883148.
  3. ^ Erbil, Yeşim; Ozluk, Yasemin; Giriş, Murat; Salmaslıoglu, Artur; Issever, Halim; Barbaros, Umut; Kapran, Yersu; Özarmağan, Selçuk; Tezelman, Serdar (2007). "Effect of Lugol Solution on Thyroid Gland Blood Flow and Microvessel Density in the Patients with Graves' Disease". The Journal of Clinical Endocrinology & Metabolism. 92 (6): 2182–2189. doi:10.1210/jc.2007-0229. PMID 17389702.
  4. ^ Pearce, Elizabeth N. (2006-06-08). "Diagnosis and management of thyrotoxicosis". BMJ. 332 (7554): 1369–1373. doi:10.1136/bmj.332.7554.1369. ISSN 0959-8138. PMC 1476727. PMID 16763249.
  5. ^ a b Furman, B. L. . www.sciencedirect.com. Archived from the original on 2023-10-03. Retrieved 2023-10-03.
  6. ^ a b Wolff, J. (March 1998). "Perchlorate and the thyroid gland". Pharmacological Reviews. 50 (1): 89–105. ISSN 0031-6997. PMID 9549759.
  7. ^ Mervish, Nancy A.; Pajak, Ashley; Teitelbaum, Susan L.; Pinney, Susan M.; Windham, Gayle C.; Kushi, Lawrence H.; Biro, Frank M.; Valentin-Blasini, Liza; Blount, Benjamin C.; Wolff, Mary S.; for the Breast Cancer and Environment Research Project (BCERP) (April 2016). "Thyroid Antagonists (Perchlorate, Thiocyanate, and Nitrate) and Childhood Growth in a Longitudinal Study of U.S. Girls". Environmental Health Perspectives. 124 (4): 542–549. doi:10.1289/ehp.1409309. ISSN 0091-6765. PMC 4829993. PMID 26151950.
  8. ^ Wyngaarden, J. B.; Stanbury, J. B.; Rapp, B. (May 1953). "The effects of iodine, perchlorate, thiocyanate, and nitrate administration upon the iodide concentrating mechanism of the rat thyroid". Endocrinology. 52 (5): 568–574. doi:10.1210/endo-52-5-568. ISSN 0013-7227. PMID 13060263.
  9. ^ Serrano-Nascimento, Caroline; Nunes, Maria Tereza (2022). "Perchlorate, nitrate, and thiocyanate: Environmental relevant NIS-inhibitors pollutants and their impact on thyroid function and human health". Frontiers in Endocrinology. 13. doi:10.3389/fendo.2022.995503. ISSN 1664-2392. PMC 9633673. PMID 36339434.
  10. ^ Lazarus, J.h. (October 1998). "The Effects of Lithium Therapy on Thyroid and Thyrotropin-Releasing Hormone". Thyroid. 8 (10): 909–913. doi:10.1089/thy.1998.8.909. ISSN 1050-7256. PMID 9827658.
  11. ^ "TG thyroglobulin [Homo sapiens (human)] – Gene – NCBI". National Center for Biotechnology Information (NCBI). Retrieved 2019-09-16.
  12. ^ Ware, Kenric; Tillery, Erika; Linder, Lauren (January 2016). "General pharmacokinetic/pharmacodynamic concepts of mood stabilizers in the treatment of bipolar disorder". The Mental Health Clinician. 6 (1): 54–61. doi:10.9740/mhc.2016.01.054. ISSN 2168-9709. PMC 6009247. PMID 29955448.
  13. ^ "Lithium Salts". The American Society of Health-System Pharmacists. from the original on 8 December 2015. Retrieved 1 December 2015.
  14. ^ Markou, K.; Georgopoulos, N.; Kyriazopoulou, V.; Vagenakis, A.g. (May 2001). "Iodine-Induced Hypothyroidism". Thyroid. 11 (5): 501–510. doi:10.1089/105072501300176462. ISSN 1050-7256. PMID 11396709.
  15. ^ a b "Iodide I-131". go.drugbank.com. Retrieved 2023-10-03.
  16. ^ Zelensky, Alex N.; Schoonakker, Mascha; Brandsma, Inger; Tijsterman, Marcel; Gent, Dik C. van; Essers, Jeroen; Kanaar, Roland (2020-01-16). "Low dose ionizing radiation strongly stimulates insertional mutagenesis in a γH2AX dependent manner". PLOS Genetics. 16 (1): e1008550. doi:10.1371/journal.pgen.1008550. ISSN 1553-7404. PMC 6964834. PMID 31945059.
  17. ^ Kim, Phillip D.; Tran, Huyen D. (2023), "I-123 Uptake", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 32644740, retrieved 2023-10-03
  18. ^ a b Schapira, Matthieu; Raaka, Bruce M.; Das, Sharmistha; Fan, Li; Totrov, Maxim; Zhou, Zhiguo; Wilson, Stephen R.; Abagyan, Ruben; Samuels, Herbert H. (2003-06-10). "Discovery of diverse thyroid hormone receptor antagonists by high-throughput docking". Proceedings of the National Academy of Sciences. 100 (12): 7354–7359. Bibcode:2003PNAS..100.7354S. doi:10.1073/pnas.1131854100. ISSN 0027-8424. PMC 165879. PMID 12777627.
  19. ^ Zambrana, J.; Zambrana, F.; Neto, F.; Gonçalves, A.; Zambrana, F.; Ushirohira, J. (2005). "Agranulocytosis with tonsillitis associated with methimazole therapy". Brazilian Journal of Otorhinolaryngology. 71 (3): 374–377. doi:10.1016/S1808-8694(15)31339-2. PMC 9450596. PMID 16446945.
  20. ^ Bahn RS, Burch HS, Cooper DS, Garber JR, Greenlee CM, Klein IL, Laurberg P, McDougall IR, et al. (July 2009). "The Role of Propylthiouracil in the Management of Graves' Disease in Adults: report of a meeting jointly sponsored by the American Thyroid Association and the Food and Drug Administration". Thyroid. 19 (7): 673–4. doi:10.1089/thy.2009.0169. PMID 19583480.
  21. ^ Pal, Partha; Ray, Sayantan; Biswas, Kaushik; Maiti, Animesh; Mukhopadhyay, Deep; George, Rintu; Mukherjee, Debabrata (September 2014). "Thyrotoxic neuropathy; an under recognized condition: A clinical vignette". Thyroid Research and Practice. 11 (3): 118. doi:10.4103/0973-0354.138559. ISSN 0973-0354.
  22. ^ Kampmann, Jens P.; Hansen, J. Mølholm (1981-12-01). "Clinical Pharmacokinetics of Antithyroid Drugs". Clinical Pharmacokinetics. 6 (6): 401–428. doi:10.2165/00003088-198106060-00001. ISSN 1179-1926. PMID 6172233. S2CID 33852149.
  23. ^ . www.sciencedirect.com. Archived from the original on 2023-10-03. Retrieved 2023-10-03.
  24. ^ Homsanit M, Sriussadaporn S, Vannasaeng S, Peerapatdit T, Nitiyanant W, Vichayanrat A (2001). "Efficacy of single daily dosage of methimazole vs. propylthiouracil in the induction of euthyroidism". Clinical Endocrinology (Oxford). 54 (3): 385–90. doi:10.1046/j.1365-2265.2001.01239.x. PMID 11298092. S2CID 24463399.
  25. ^ Glinoer D, de Nayer P, Bex M (2001). "Effects of l-thyroxine administration, TSH-receptor antibodies and smoking on the risk of recurrence in Graves' hyperthyroidism treated with antithyroid drugs: a double-blind prospective randomized study". Eur. J. Endocrinol. 144 (5): 475–83. doi:10.1530/eje.0.1440475. PMID 11331213.

External links edit

April 12, 2024
antithyroid, agent, antithyroid, agent, hormone, inhibitor, acting, upon, thyroid, hormones, main, antithyroid, drugs, carbimazole, methimazole, propylthiouracil, less, common, antithyroid, agent, potassium, perchlorate, contents, classification, based, mechan. An antithyroid agent is a hormone inhibitor acting upon thyroid hormones The main antithyroid drugs are carbimazole in the UK methimazole in the US and propylthiouracil PTU A less common antithyroid agent is potassium perchlorate Contents 1 Classification based on mechanisms of action 1 1 Thyroid hormone synthesis inhbitors 1 2 Iodide uptake inhibitors 1 3 Thyroid hormone release inhibitors 1 4 Excess iodine 1 5 Iodine radiopharmaceuticals 1 6 Thyroid hormone receptor antagonists 2 Adverse effects 3 Graves disease 4 See also 5 Notes 6 References 7 External linksClassification based on mechanisms of action editThe mechanisms of action of antithyroid drugs are not completely understood Based on their mechanisms of action the drugs are classified into following six classes Thyroid hormone synthesis inhbitors edit These drugs probably inhibit the enzyme thyroid peroxidase a k a thyroperoxidase decreasing iodide oxidation iodination of tyrosyl residues in thyroglobulin and coupling of iodotyrosyl and iodothyronyl residues 1 It is thought that they inhibit the thyroperoxidase catalyzed oxidation reactions by acting as substrates for the postulated peroxidase iodine complex thus competitively inhibiting the interaction with the amino acid tyrosine The most common drugs in this class are thioamides which include propylthiouracil methimazole and its prodrug carbimazole Additionally propylthiouracil may reduce the de iodination of thyroxine tetraiodothyronine T4 into triiodothyronine T3 in peripheral tissues 2 Lugol s iodine is used to temporarily block thyroid hormone synthesis before surgeries 3 It is also used to treat patients with thyroid storm or more commonly to reduce thyroid vascularity before thyroidectomy surgical removal of the thyroid gland 4 Iodide uptake inhibitors edit They decrease uptake of iodide ions I into follicular cells of the thyroid gland Since their molecules have structural similarities with the iodide ion they compete with iodide for being transported by the sodium iodide symporter which is a transporter protein that co transports Na and I ions Iodide transport is a key step in the biosynthesis of the thyroid hormones T4 and T3 5 6 For example potassium perchlorate competitively inhibits the active iodide transport mechanism in the thyroid gland which has the capacity to selectively concentrate iodide against a large concentration gradient 5 6 Besides perchlorates other examples of iodide uptake inhibitors include pertechnetates thiocyanates nitrates 7 These drugs are no longer used due to high toxicity and adverse effects 8 9 Thyroid hormone release inhibitors edit They inhibit release secretion of thyroid hormones by the thyroid gland The most studied drug in this class is lithium which inhibits thyroid hormone secretion by inhibiting iodotyrosine coupling thyroidal iodide uptake and alteration in structure of thyroglobulin 10 a protein which acts as a substrate for the synthesis of thyroid hormones and storage of inactive forms of T3 T4 and iodine within the lumen of thyroid follicular cells 11 Since lithium is neither metabolized nor protein bound its bioavailability usually is close to 100 12 Hence there are risks of serious side effects such as lithium toxicity hypothyroidism and diabetes insipidus 13 Excess iodine edit Excessive iodine intake can temporarily inhibit production of thyroid hormones This occurs because of the Wolff Chaikoff effect which is a phenomenon of rejection of large quantities of iodine by the thyroid gland therefore preventing it from synthesizing large quantities of thyroid hormones 14 Iodine radiopharmaceuticals edit Main articles Isotopes of iodine and radiopharmaceutical They are radioisotopes of iodine In small doses when they are taken up by overactive thyroid follicular cells they emit small amounts of beta radiation that destroys not all but many thyroid follicular cells thereby reducing thyroid hormone production 15 This is a form of targeted therapy for hyperthyroidism Since even low levels of ionizing radiation are highly mutagenic and can cause cancer 16 less toxic iodine isotopes such as iodine 123 17 are more commonly used in nuclear imaging while iodine 131 is used for its cytolytic cell destroying effects in hyperthyroidism and thyroid tumors 15 Thyroid hormone receptor antagonists edit Also called TR antagonists they inhibit action of thyroid hormones by blocking TR receptors thyroid hormone receptors Antagonist 1 850 and its derivatives have been found to be coactivator interaction inhibitors which interfere with the interaction between TR receptors and coactivator proteins such as nuclear hormone receptor coregulator NRC As a result the receptors are unable to recruit coactivators causing stoppage of transcription of target genes thereby preventing activation of TR receptors ultimately leading to inhibition of effects of thyroid hormones because they can bind to only inactive TR receptors and these receptors can t be activated in presence of TR antagonists 18 Antagonist 1 850 has also been found to inhibit binding of 125I T3 a to TRs in intact GH4 cells 18 Adverse effects editThe most dangerous side effect is agranulocytosis 1 250 more in PTU this is an idiosyncratic reaction which generally resolves on cessation of drug It occurs in about 0 2 to 0 3 of cases treated with antithyroid drugs 19 Other side effects include granulocytopenia dose dependent which improves on cessation of the drug and aplastic anemia and in case of propylthiouracil severe fulminant liver failure 20 Patients on these medications should see a doctor if they develop sore throat or fever The most common side effects are rash and peripheral neuritis 21 These drugs also cross the placenta and are secreted in breast milk 22 Graves disease editIn Graves disease treatment with antithyroid medications must be given for six months to two years in order to be effective Even then upon cessation of the drugs the hyperthyroid state may recur Side effects of the antithyroid medications include a potentially fatal reduction in the level of white blood cells A randomized control trial testing single dose treatment for Graves found methimazole achieved euthyroidism normal thyroid function that occurs within normal serum levels of TSH and T4 23 more effectively after 12 weeks than did propylthiouracil 77 1 on methimazole 15 mg vs 19 4 in the propylthiouracil 150 mg groups 24 But generally both drugs are considered equivalent A study has shown no difference in outcome for adding thyroxine to antithyroid medication and continuing thyroxine versus placebo after antithyroid medication withdrawal However two markers were found that can help predict the risk of recurrence These two markers are an elevated level of thyroid stimulating hormone receptor antibodies TSHR Ab and smoking A positive TSHR Ab at the end of antithyroid drug treatment increases the risk of recurrence to 90 sensitivity 39 specificity 98 a negative TSHR Ab at the end of antithyroid drug treatment is associated with a 78 chance of remaining in remission Smoking was shown to have an impact independent to a positive TSHR Ab 25 Competitive antagonists of thyroid stimulating hormone receptors are currently being investigated as a possible treatment for Grave s disease See also editH03B code of antithyroid preparationsNotes edit 125I T3 is a radiopharmaceutical formulation of triiodothyronine having iodine 125 atoms instead of iodine References edit Thioamide an overview ScienceDirect Topics www sciencedirect com Archived from the original on 2023 09 27 Retrieved 2023 10 03 Manna D Roy G Mugesh G 2013 Antithyroid Drugs and their Analogues Synthesis Structure and Mechanism of Action Acc Chem Res 46 11 2706 15 doi 10 1021 ar4001229 PMID 23883148 Erbil Yesim Ozluk Yasemin Giris Murat Salmaslioglu Artur Issever Halim Barbaros Umut Kapran Yersu Ozarmagan Selcuk Tezelman Serdar 2007 Effect of Lugol Solution on Thyroid Gland Blood Flow and Microvessel Density in the Patients with Graves Disease The Journal of Clinical Endocrinology amp Metabolism 92 6 2182 2189 doi 10 1210 jc 2007 0229 PMID 17389702 Pearce Elizabeth N 2006 06 08 Diagnosis and management of thyrotoxicosis BMJ 332 7554 1369 1373 doi 10 1136 bmj 332 7554 1369 ISSN 0959 8138 PMC 1476727 PMID 16763249 a b Furman B L Potassium Perchlorate an overview ScienceDirect Topics www sciencedirect com Archived from the original on 2023 10 03 Retrieved 2023 10 03 a b Wolff J March 1998 Perchlorate and the thyroid gland Pharmacological Reviews 50 1 89 105 ISSN 0031 6997 PMID 9549759 Mervish Nancy A Pajak Ashley Teitelbaum Susan L Pinney Susan M Windham Gayle C Kushi Lawrence H Biro Frank M Valentin Blasini Liza Blount Benjamin C Wolff Mary S for the Breast Cancer and Environment Research Project BCERP April 2016 Thyroid Antagonists Perchlorate Thiocyanate and Nitrate and Childhood Growth in a Longitudinal Study of U S Girls Environmental Health Perspectives 124 4 542 549 doi 10 1289 ehp 1409309 ISSN 0091 6765 PMC 4829993 PMID 26151950 Wyngaarden J B Stanbury J B Rapp B May 1953 The effects of iodine perchlorate thiocyanate and nitrate administration upon the iodide concentrating mechanism of the rat thyroid Endocrinology 52 5 568 574 doi 10 1210 endo 52 5 568 ISSN 0013 7227 PMID 13060263 Serrano Nascimento Caroline Nunes Maria Tereza 2022 Perchlorate nitrate and thiocyanate Environmental relevant NIS inhibitors pollutants and their impact on thyroid function and human health Frontiers in Endocrinology 13 doi 10 3389 fendo 2022 995503 ISSN 1664 2392 PMC 9633673 PMID 36339434 Lazarus J h October 1998 The Effects of Lithium Therapy on Thyroid and Thyrotropin Releasing Hormone Thyroid 8 10 909 913 doi 10 1089 thy 1998 8 909 ISSN 1050 7256 PMID 9827658 TG thyroglobulin Homo sapiens human Gene NCBI National Center for Biotechnology Information NCBI Retrieved 2019 09 16 Ware Kenric Tillery Erika Linder Lauren January 2016 General pharmacokinetic pharmacodynamic concepts of mood stabilizers in the treatment of bipolar disorder The Mental Health Clinician 6 1 54 61 doi 10 9740 mhc 2016 01 054 ISSN 2168 9709 PMC 6009247 PMID 29955448 Lithium Salts The American Society of Health System Pharmacists Archived from the original on 8 December 2015 Retrieved 1 December 2015 Markou K Georgopoulos N Kyriazopoulou V Vagenakis A g May 2001 Iodine Induced Hypothyroidism Thyroid 11 5 501 510 doi 10 1089 105072501300176462 ISSN 1050 7256 PMID 11396709 a b Iodide I 131 go drugbank com Retrieved 2023 10 03 Zelensky Alex N Schoonakker Mascha Brandsma Inger Tijsterman Marcel Gent Dik C van Essers Jeroen Kanaar Roland 2020 01 16 Low dose ionizing radiation strongly stimulates insertional mutagenesis in a gH2AX dependent manner PLOS Genetics 16 1 e1008550 doi 10 1371 journal pgen 1008550 ISSN 1553 7404 PMC 6964834 PMID 31945059 Kim Phillip D Tran Huyen D 2023 I 123 Uptake StatPearls Treasure Island FL StatPearls Publishing PMID 32644740 retrieved 2023 10 03 a b Schapira Matthieu Raaka Bruce M Das Sharmistha Fan Li Totrov Maxim Zhou Zhiguo Wilson Stephen R Abagyan Ruben Samuels Herbert H 2003 06 10 Discovery of diverse thyroid hormone receptor antagonists by high throughput docking Proceedings of the National Academy of Sciences 100 12 7354 7359 Bibcode 2003PNAS 100 7354S doi 10 1073 pnas 1131854100 ISSN 0027 8424 PMC 165879 PMID 12777627 Zambrana J Zambrana F Neto F Goncalves A Zambrana F Ushirohira J 2005 Agranulocytosis with tonsillitis associated with methimazole therapy Brazilian Journal of Otorhinolaryngology 71 3 374 377 doi 10 1016 S1808 8694 15 31339 2 PMC 9450596 PMID 16446945 Bahn RS Burch HS Cooper DS Garber JR Greenlee CM Klein IL Laurberg P McDougall IR et al July 2009 The Role of Propylthiouracil in the Management of Graves Disease in Adults report of a meeting jointly sponsored by the American Thyroid Association and the Food and Drug Administration Thyroid 19 7 673 4 doi 10 1089 thy 2009 0169 PMID 19583480 Pal Partha Ray Sayantan Biswas Kaushik Maiti Animesh Mukhopadhyay Deep George Rintu Mukherjee Debabrata September 2014 Thyrotoxic neuropathy an under recognized condition A clinical vignette Thyroid Research and Practice 11 3 118 doi 10 4103 0973 0354 138559 ISSN 0973 0354 Kampmann Jens P Hansen J Molholm 1981 12 01 Clinical Pharmacokinetics of Antithyroid Drugs Clinical Pharmacokinetics 6 6 401 428 doi 10 2165 00003088 198106060 00001 ISSN 1179 1926 PMID 6172233 S2CID 33852149 Euthyroidism an overview ScienceDirect Topics www sciencedirect com Archived from the original on 2023 10 03 Retrieved 2023 10 03 Homsanit M Sriussadaporn S Vannasaeng S Peerapatdit T Nitiyanant W Vichayanrat A 2001 Efficacy of single daily dosage of methimazole vs propylthiouracil in the induction of euthyroidism Clinical Endocrinology Oxford 54 3 385 90 doi 10 1046 j 1365 2265 2001 01239 x PMID 11298092 S2CID 24463399 Glinoer D de Nayer P Bex M 2001 Effects of l thyroxine administration TSH receptor antibodies and smoking on the risk of recurrence in Graves hyperthyroidism treated with antithyroid drugs a double blind prospective randomized study Eur J Endocrinol 144 5 475 83 doi 10 1530 eje 0 1440475 PMID 11331213 External links editAntithyroid agents at the U S National Library of Medicine Medical Subject Headings MeSH Retrieved from https en wikipedia org w index php title Antithyroid agent amp oldid 1190260440, wikipedia, wiki, book, books, library,

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