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Medullary thyroid cancer

April 14, 2024

Medullary thyroid cancer is a form of thyroid carcinoma which originates from the parafollicular cells (C cells), which produce the hormone calcitonin.[1] Medullary tumors are the third most common of all thyroid cancers and together make up about 3% of all thyroid cancer cases.[2] MTC was first characterized in 1959.[3]

Medullary thyroid cancer
Other namesMTC
Micrograph of medullary thyroid carcinoma with amyloid deposition (left of image). Near normal thyroid follicles are also seen (right of image). H&E stain.
SpecialtyENT surgery

Approximately 25% of medullary thyroid cancer cases are genetic in nature, caused by a mutation in the RET proto-oncogene. When MTC occurs by itself it is termed sporadic medullary thyroid cancer. Medullary thyroid cancer is seen in people with multiple endocrine neoplasia type 2A and 2B. When medullary thyroid cancer due to a hereditary genetic disorder occurs without other endocrine tumours it is termed familial medullary thyroid cancer.

Signs and symptoms edit

The major clinical symptom of metastatic medullary thyroid carcinoma is diarrhea; occasionally a patient will have flushing episodes. Both occur particularly with liver metastasis, and either symptom may be the first manifestation of the disease. The flushing that occurs in medullary thyroid carcinoma is indistinguishable from that associated with carcinoid syndrome. In MTC, the flushing, diarrhea, and itching (pruritus) are all caused by elevated levels of calcitonin gene products (calcitonin or calcitonin gene-related peptide).[4] By comparison, the flushing and diarrhea observed in carcinoid syndrome is caused by elevated levels of circulating serotonin.

Medullary thyroid carcinoma may also produce a thyroid nodule and enlarged cervical lymph nodes.[4]

Sites of spread of medullary thyroid carcinoma include local lymph nodes in the neck, lymph nodes in the central portion of the chest (mediastinum), liver, lung, and bone. Spread to other sites such as skin or brain occurs but is uncommon.

Genetics edit

Mutations (DNA changes) in the RET proto-oncogene, located on chromosome 10, lead to the expression of a mutated receptor tyrosine kinase protein, termed RET (REarranged during Transfection). RET is involved in the regulation of cell growth and development and its germline mutation is responsible for nearly all cases of hereditary or familial medullary thyroid carcinoma. Its germline mutation may also be responsible for the development of hyperparathyroidism and pheochromocytoma. Hereditary medullary thyroid cancer is inherited as an autosomal dominant trait, meaning that each child of an affected parent has a 50% probability of inheriting the mutant RET proto-oncogene from the affected parent. DNA analysis makes it possible to identify children who carry the mutant gene; surgical removal of the thyroid in children who carry the mutant gene is curative if the entire thyroid gland is removed at an early age, before there is spread of the tumor. The parathyroid tumors and pheochromocytomas are removed when they cause clinical symptomatology. Hereditary medullary thyroid carcinoma or multiple endocrine neoplasia (MEN2) accounts for approximately 25% of all medullary thyroid carcinomas.

Seventy-five percent of medullary thyroid carcinoma occurs in individuals without an identifiable family history and is assigned the term "sporadic". Individuals who develop sporadic medullary thyroid carcinoma tend to be older and have more extensive disease at the time of initial presentation than those with a family history (screening is likely to be initiated at an early age in the hereditary form). Approximately 25-60% of sporadic medullary thyroid carcinomas have a somatic mutation (one that occurs within a single "parafollicular" cell) of the RET proto-oncogene. This mutation is presumed to be the initiating event, although there could be other as yet unidentified causes.

Markers edit

While the increased serum concentration of calcitonin is not harmful, it is useful as a marker which can be tested in blood.[5]

A second marker, carcinoembryonic antigen (CEA), also produced by medullary thyroid carcinoma, is released into the blood and it is useful as a serum or blood tumor marker. In general, measurement of serum CEA is less sensitive than serum calcitonin for detecting the presence of a tumor, but has less minute to minute variability and is therefore useful as an indicator of tumor mass.

Diagnosis edit

 
Medullary thyroid carcinoma on ultrasound with typical small calcifications (arrows)

Diagnosis is primarily performed via fine needle aspiration of the lesion of the thyroid to distinguish it from other types of thyroid lesions.[6] Microscopic examination will show an amyloid stroma with hyperplasia of parafollicular cells.

A recent Cochrane systematic review assessed the diagnostic accuracy of basal and stimulated calcitonin for Medullary Thyroid Carcinoma.[7] Although both basal and combined basal and stimulated calcitonin testing presented high accuracy (sensitivity: between 82% and 100%; specificity: between 97.2% and 100%), these results had a high risk of bias due to design flaws of included studies.[7] Overall, the value of routine testing of calcitonin for diagnosis and prognosis of Medullary Thyroid Carcinoma remains uncertain and questionable.[7]

Treatment edit

Surgery and radiation therapy have been the major treatments for medullary thyroid carcinoma. A plasma level of metanephrines should be checked before surgical thyroidectomy takes place to evaluate for the presence of pheochromocytoma since 25% of people found to have medullary thyroid cancer have the inherited form from the MEN2A syndrome. Undiagnosed pheochromocytoma leads to a very high intraoperative risk of hypertensive crisis and, potentially, death.

Surgery edit

 
A surgery for MTC showing the central lymph nodes and thyroid gland removed

A total thyroidectomy with bilateral neck dissection is the gold standard for treating medullary thyroid cancer, and is the most definitive means of achieving a cure in patients without distant metastases or extensive nodal involvement. Risks of surgery include loss of vocal control, irreparable nerve damage, death or the need for second operation to clean out residual diseased lymph nodes left behind if the sentinel node biopsy was positive for cancerous spread. Extensive surgery can be effective when the condition is detected early, but a risk for recurrence remains, particularly in patients with multiple positive lymph nodes or extracapsular invasion.[1][8] About half of patients have metastasis to regional lymph nodes at the time of diagnosis.[4]

The European Society of Endocrine Surgeons has published recommendations for managing this condition in gene carriers.[9] The timing of surgery depends on the type of mutation present. For those in the highest risk group, surgery is recommended in the first year of life. In lower risk cases surgery may be delayed up to the age of ten years, the precise timing depending on the mutation and other factors.

Radiation edit

External beam radiotherapy is recommended when there is a high risk of regional recurrence, even after optimum surgical treatment.[10][11] In this study, patients treated with external beam radiation were compared to a control group. Disease control with radiation was far superior in the group receiving radiation. The authors of the study [14] wrote: "in 40 high risk patients (microscopic residual disease, extraglandular invasion, or lymph node involvement), the local/regional relapse free rate was 86% at 10 years with postoperative external beam radiation (25 patients), and 52% for those with no postoperative external radiation (p = 0.049). To optimize local/regional tumor control, we therefore continue to advise external beam radiation in patients at high risk of local/regional relapse."

Unlike other differentiated thyroid carcinoma, there is no role for radioiodine treatment in medullary-type disease.[12]

Protein kinase inhibitors edit

Clinical trials of protein kinase inhibitors,[13] which block the abnormal kinase proteins involved in the development and growth of medullary cancer cells, showed clear evidence of response in 10-30% of patients. In the majority of responders there has been less than a 30% decrease in tumor mass, yet the responses have been durable; responses have been stable for periods exceeding 3 years. The major side effects of this class of drug include hypertension, nausea, diarrhea, some cardiac electrical abnormalities, and thrombotic or bleeding episodes.

Vandetanib, trade name Caprelsa, was the first drug (April 2011) to be approved by US Food and Drug Administration (FDA) for treatment of late-stage (metastatic) medullary thyroid cancer in adult patients who are ineligible for surgery.[14]

Cabozantinib, trade name Cometriq, was granted marketing approval (November 2012) by the U.S. FDA for this indication.[15] Cabozantinib which is a potent inhibitor of RET, MET and VEGF was evaluated in a double-blind placebo controlled trial. It was shown to improve overall survival by 5 months for the treated cohort vs. placebo, which was not statistically significant. However, cabozantinib was particularly effective in patients with the RET M918T mutation, extending overall survival by roughly 2 years, doubling survival vs. untreated patient (4 years vs. 2 year). Treatment with cabozantinib did require many dose reduction to mitigate side effects. It has been suggested that the trial dose of 140 mg was excessive, particularly in lower body mass patients. Ongoing trials have been scheduled to identify more optimal dosing regimes. Activity has been observed, in practice at doses of 1.2 mg/kg.

Prognosis edit

Depending on source, the overall 5-year survival rate for medullary thyroid cancer is 80%,[16] 83%[17] or 86%,[6] and the 10-year survival rate is 75%.[16]

By overall cancer staging into stages I to IV, the 5-year survival rate is 100% at stage I, 98% at stage II, 81% at stage III and 28% at stage IV.[18] The prognosis of MTC is poorer than that of follicular and papillary thyroid cancer when it has metastasized (spread) beyond the thyroid gland.

The prognostic value of measuring calcitonin and carcinoembryonic antigen (CEA) concentrations in the blood was studied in 65 MTC patients who had abnormal calcitonin levels after surgery (total thyroidectomy and lymph node dissection).[19] The prognosis correlated with the rate at which the postoperative calcitonin concentration doubles, termed the calcitonin doubling time (CDT), rather than the pre- or postoperative absolute calcitonin level:

  • CDT less than 6 months: 3 patients out of 12 (25%) survived 5 years. 1 patient out of 12 (8%) survived 10 years. All died within 6 months to 13.3 years.
  • CDT between 6 months and 2 years: 11 patients out of 12 (92%) survived 5 years. 3 patients out of 8 (37%) survived 10 years. 4 patients out of 12 (25%) survived to the end of the study.
  • CDT more than 2 years: 41 patients out of 41 (100%) were alive at the end of the study. These included 1 patient whose calcitonin was stable, and 11 patients who had decreasing calcitonin levels.

The calcitonin doubling time was a better predictor of MTC survival than CEA[19] but following both tests is recommended.[10][20]

References edit

  1. ^ a b Hu MI, Vassilopoulou-Sellin R, Lustig R, Lamont JP. "Thyroid and Parathyroid Cancers" in Pazdur R, Wagman LD, Camphausen KA, Hoskins WJ (Eds) Cancer Management: A Multidisciplinary Approach. 11 ed. 2008.
  2. ^ Stamatakos M, Paraskeva P, Stefanaki C, Katsaronis P, Lazaris A, Safioleas K, Kontzoglou K (January 2011). "Medullary thyroid carcinoma: The third most common thyroid cancer reviewed". Oncol Lett. 2 (1): 49–53. doi:10.3892/ol.2010.223. PMC 3412473. PMID 22870127.
  3. ^ Dionigi G, Bianchi V, Rovera F, et al. (2007). "Medullary thyroid carcinoma: surgical treatment advances". Expert Rev Anticancer Ther. 7 (6): 877–85. doi:10.1586/14737140.7.6.877. PMID 17555398. S2CID 37519975.
  4. ^ a b c Goldman L (2011). Goldman's Cecil Medicine (24th ed.). Philadelphia: Elsevier Saunders. pp. e76. ISBN 978-1437727883.
  5. ^ Fragu P (2007). "Calcitonin's fantastic voyage: from hormone to marker of a genetic disorder". Gesnerus. 64 (1–2): 69–92. doi:10.1163/22977953-0640102004. PMID 17982960.
  6. ^ a b National Cancer Institute > Medullary Thyroid Cancer Last Modified: 12/22/2010
  7. ^ a b c Verbeek HH, de Groot JW, Sluiter WJ, Muller Kobold AC, van den Heuvel ER, Plukker JT, Links TP, et al. (Cochrane Metabolic and Endocrine Disorders Group) (March 2020). "Calcitonin testing for detection of medullary thyroid cancer in people with thyroid nodules". The Cochrane Database of Systematic Reviews. 2020 (3): CD010159. doi:10.1002/14651858.CD010159.pub2. PMC 7075519. PMID 32176812.
  8. ^ Schlumberger M, Carlomagno F, Baudin E, Bidart JM, Santoro M (2008). "New therapeutic approaches to treat medullary thyroid carcinoma". Nat Clin Pract Endocrinol Metab. 4 (1): 22–32. doi:10.1038/ncpendmet0717. PMID 18084343. S2CID 25818628.
  9. ^ Niederle B, Sebag F, Brauckhoff M (2013) Timing and extent of thyroid surgery for gene carriers of hereditary C cell disease-a consensus statement of the European Society of Endocrine Surgeons (ESES).Langenbecks Arch Surg
  10. ^ a b (PDF). NCCN guidelines. National Comprehensive Cancer Network. Archived from the original (PDF) on 25 September 2006.
  11. ^ Brierley J, Tsang R, Simpson WJ, Gospodarowicz M, Sutcliffe S, Panzarella T (1996). "Medullary thyroid cancer: analyses of survival and prognostic factors and the role of radiation therapy in local control". Thyroid. 6 (4): 305–10. doi:10.1089/thy.1996.6.305. PMID 8875751.
  12. ^ Quayle FJ, Moley JF (2005). "Medullary thyroid carcinoma: including MEN 2A and MEN 2B syndromes". J Surg Oncol. 89 (3): 122–9. doi:10.1002/jso.20184. PMID 15719378. S2CID 31436486.
  13. ^ . Archived from the original on 2007-12-12. Retrieved 2007-12-21.
  14. ^ "FDA approves new treatment for rare form of thyroid cancer". Food and Drug Administration. Retrieved 7 April 2011.
  15. ^ "FDA approves Cometriq to treat rare type of thyroid cancer". Food and Drug Administration. Retrieved 29 November 2012.
  16. ^ a b Numbers from National Cancer Database in the US, from Page 10 in: F. Grünwald; Biersack, H. J.; Grںunwald, F. (2005). Thyroid cancer. Berlin: Springer. ISBN 978-3-540-22309-2.
  17. ^ Barbet J, Campion L, Kraeber-Bodéré F, Chatal JF (November 2005). "Prognostic impact of serum calcitonin and carcinoembryonic antigen doubling-times in patients with medullary thyroid carcinoma". The Journal of Clinical Endocrinology and Metabolism. 90 (11): 6077–6084. doi:10.1210/jc.2005-0044. PMID 16091497.
  18. ^ cancer.org > Thyroid Cancer October 18, 2013, at the Wayback Machine By the American Cancer Society. In turn citing: AJCC Cancer Staging Manual (7th ed).
  19. ^ a b Barbet J, Campion L, Kraeber-Bodéré F, Chatal JF (2005). "Prognostic impact of serum calcitonin and carcinoembryonic antigen doubling-times in patients with medullary thyroid carcinoma". J. Clin. Endocrinol. Metab. 90 (11): 6077–84. doi:10.1210/jc.2005-0044. PMID 16091497.
  20. ^ "ASCO Self-Evaluation Program (SEP)". American Society of Clinical Oncology (ASCO).

External links edit

April 14, 2024
medullary, thyroid, cancer, form, thyroid, carcinoma, which, originates, from, parafollicular, cells, cells, which, produce, hormone, calcitonin, medullary, tumors, third, most, common, thyroid, cancers, together, make, about, thyroid, cancer, cases, first, ch. Medullary thyroid cancer is a form of thyroid carcinoma which originates from the parafollicular cells C cells which produce the hormone calcitonin 1 Medullary tumors are the third most common of all thyroid cancers and together make up about 3 of all thyroid cancer cases 2 MTC was first characterized in 1959 3 Medullary thyroid cancerOther namesMTCMicrograph of medullary thyroid carcinoma with amyloid deposition left of image Near normal thyroid follicles are also seen right of image H amp E stain SpecialtyENT surgeryApproximately 25 of medullary thyroid cancer cases are genetic in nature caused by a mutation in the RET proto oncogene When MTC occurs by itself it is termed sporadic medullary thyroid cancer Medullary thyroid cancer is seen in people with multiple endocrine neoplasia type 2A and 2B When medullary thyroid cancer due to a hereditary genetic disorder occurs without other endocrine tumours it is termed familial medullary thyroid cancer Contents 1 Signs and symptoms 2 Genetics 2 1 Markers 3 Diagnosis 4 Treatment 4 1 Surgery 4 2 Radiation 4 3 Protein kinase inhibitors 5 Prognosis 6 References 7 External linksSigns and symptoms editThe major clinical symptom of metastatic medullary thyroid carcinoma is diarrhea occasionally a patient will have flushing episodes Both occur particularly with liver metastasis and either symptom may be the first manifestation of the disease The flushing that occurs in medullary thyroid carcinoma is indistinguishable from that associated with carcinoid syndrome In MTC the flushing diarrhea and itching pruritus are all caused by elevated levels of calcitonin gene products calcitonin or calcitonin gene related peptide 4 By comparison the flushing and diarrhea observed in carcinoid syndrome is caused by elevated levels of circulating serotonin Medullary thyroid carcinoma may also produce a thyroid nodule and enlarged cervical lymph nodes 4 Sites of spread of medullary thyroid carcinoma include local lymph nodes in the neck lymph nodes in the central portion of the chest mediastinum liver lung and bone Spread to other sites such as skin or brain occurs but is uncommon Genetics editMutations DNA changes in the RET proto oncogene located on chromosome 10 lead to the expression of a mutated receptor tyrosine kinase protein termed RET REarranged during Transfection RET is involved in the regulation of cell growth and development and its germline mutation is responsible for nearly all cases of hereditary or familial medullary thyroid carcinoma Its germline mutation may also be responsible for the development of hyperparathyroidism and pheochromocytoma Hereditary medullary thyroid cancer is inherited as an autosomal dominant trait meaning that each child of an affected parent has a 50 probability of inheriting the mutant RET proto oncogene from the affected parent DNA analysis makes it possible to identify children who carry the mutant gene surgical removal of the thyroid in children who carry the mutant gene is curative if the entire thyroid gland is removed at an early age before there is spread of the tumor The parathyroid tumors and pheochromocytomas are removed when they cause clinical symptomatology Hereditary medullary thyroid carcinoma or multiple endocrine neoplasia MEN2 accounts for approximately 25 of all medullary thyroid carcinomas Seventy five percent of medullary thyroid carcinoma occurs in individuals without an identifiable family history and is assigned the term sporadic Individuals who develop sporadic medullary thyroid carcinoma tend to be older and have more extensive disease at the time of initial presentation than those with a family history screening is likely to be initiated at an early age in the hereditary form Approximately 25 60 of sporadic medullary thyroid carcinomas have a somatic mutation one that occurs within a single parafollicular cell of the RET proto oncogene This mutation is presumed to be the initiating event although there could be other as yet unidentified causes Markers edit While the increased serum concentration of calcitonin is not harmful it is useful as a marker which can be tested in blood 5 A second marker carcinoembryonic antigen CEA also produced by medullary thyroid carcinoma is released into the blood and it is useful as a serum or blood tumor marker In general measurement of serum CEA is less sensitive than serum calcitonin for detecting the presence of a tumor but has less minute to minute variability and is therefore useful as an indicator of tumor mass Diagnosis edit nbsp Medullary thyroid carcinoma on ultrasound with typical small calcifications arrows Diagnosis is primarily performed via fine needle aspiration of the lesion of the thyroid to distinguish it from other types of thyroid lesions 6 Microscopic examination will show an amyloid stroma with hyperplasia of parafollicular cells A recent Cochrane systematic review assessed the diagnostic accuracy of basal and stimulated calcitonin for Medullary Thyroid Carcinoma 7 Although both basal and combined basal and stimulated calcitonin testing presented high accuracy sensitivity between 82 and 100 specificity between 97 2 and 100 these results had a high risk of bias due to design flaws of included studies 7 Overall the value of routine testing of calcitonin for diagnosis and prognosis of Medullary Thyroid Carcinoma remains uncertain and questionable 7 Treatment editSurgery and radiation therapy have been the major treatments for medullary thyroid carcinoma A plasma level of metanephrines should be checked before surgical thyroidectomy takes place to evaluate for the presence of pheochromocytoma since 25 of people found to have medullary thyroid cancer have the inherited form from the MEN2A syndrome Undiagnosed pheochromocytoma leads to a very high intraoperative risk of hypertensive crisis and potentially death Surgery edit nbsp A surgery for MTC showing the central lymph nodes and thyroid gland removedA total thyroidectomy with bilateral neck dissection is the gold standard for treating medullary thyroid cancer and is the most definitive means of achieving a cure in patients without distant metastases or extensive nodal involvement Risks of surgery include loss of vocal control irreparable nerve damage death or the need for second operation to clean out residual diseased lymph nodes left behind if the sentinel node biopsy was positive for cancerous spread Extensive surgery can be effective when the condition is detected early but a risk for recurrence remains particularly in patients with multiple positive lymph nodes or extracapsular invasion 1 8 About half of patients have metastasis to regional lymph nodes at the time of diagnosis 4 The European Society of Endocrine Surgeons has published recommendations for managing this condition in gene carriers 9 The timing of surgery depends on the type of mutation present For those in the highest risk group surgery is recommended in the first year of life In lower risk cases surgery may be delayed up to the age of ten years the precise timing depending on the mutation and other factors Radiation edit External beam radiotherapy is recommended when there is a high risk of regional recurrence even after optimum surgical treatment 10 11 In this study patients treated with external beam radiation were compared to a control group Disease control with radiation was far superior in the group receiving radiation The authors of the study 14 wrote in 40 high risk patients microscopic residual disease extraglandular invasion or lymph node involvement the local regional relapse free rate was 86 at 10 years with postoperative external beam radiation 25 patients and 52 for those with no postoperative external radiation p 0 049 To optimize local regional tumor control we therefore continue to advise external beam radiation in patients at high risk of local regional relapse Unlike other differentiated thyroid carcinoma there is no role for radioiodine treatment in medullary type disease 12 Protein kinase inhibitors edit Clinical trials of protein kinase inhibitors 13 which block the abnormal kinase proteins involved in the development and growth of medullary cancer cells showed clear evidence of response in 10 30 of patients In the majority of responders there has been less than a 30 decrease in tumor mass yet the responses have been durable responses have been stable for periods exceeding 3 years The major side effects of this class of drug include hypertension nausea diarrhea some cardiac electrical abnormalities and thrombotic or bleeding episodes Vandetanib trade name Caprelsa was the first drug April 2011 to be approved by US Food and Drug Administration FDA for treatment of late stage metastatic medullary thyroid cancer in adult patients who are ineligible for surgery 14 Cabozantinib trade name Cometriq was granted marketing approval November 2012 by the U S FDA for this indication 15 Cabozantinib which is a potent inhibitor of RET MET and VEGF was evaluated in a double blind placebo controlled trial It was shown to improve overall survival by 5 months for the treated cohort vs placebo which was not statistically significant However cabozantinib was particularly effective in patients with the RET M918T mutation extending overall survival by roughly 2 years doubling survival vs untreated patient 4 years vs 2 year Treatment with cabozantinib did require many dose reduction to mitigate side effects It has been suggested that the trial dose of 140 mg was excessive particularly in lower body mass patients Ongoing trials have been scheduled to identify more optimal dosing regimes Activity has been observed in practice at doses of 1 2 mg kg Prognosis editDepending on source the overall 5 year survival rate for medullary thyroid cancer is 80 16 83 17 or 86 6 and the 10 year survival rate is 75 16 By overall cancer staging into stages I to IV the 5 year survival rate is 100 at stage I 98 at stage II 81 at stage III and 28 at stage IV 18 The prognosis of MTC is poorer than that of follicular and papillary thyroid cancer when it has metastasized spread beyond the thyroid gland The prognostic value of measuring calcitonin and carcinoembryonic antigen CEA concentrations in the blood was studied in 65 MTC patients who had abnormal calcitonin levels after surgery total thyroidectomy and lymph node dissection 19 The prognosis correlated with the rate at which the postoperative calcitonin concentration doubles termed the calcitonin doubling time CDT rather than the pre or postoperative absolute calcitonin level CDT less than 6 months 3 patients out of 12 25 survived 5 years 1 patient out of 12 8 survived 10 years All died within 6 months to 13 3 years CDT between 6 months and 2 years 11 patients out of 12 92 survived 5 years 3 patients out of 8 37 survived 10 years 4 patients out of 12 25 survived to the end of the study CDT more than 2 years 41 patients out of 41 100 were alive at the end of the study These included 1 patient whose calcitonin was stable and 11 patients who had decreasing calcitonin levels The calcitonin doubling time was a better predictor of MTC survival than CEA 19 but following both tests is recommended 10 20 References edit a b Hu MI Vassilopoulou Sellin R Lustig R Lamont JP Thyroid and Parathyroid Cancers in Pazdur R Wagman LD Camphausen KA Hoskins WJ Eds Cancer Management A Multidisciplinary Approach 11 ed 2008 Stamatakos M Paraskeva P Stefanaki C Katsaronis P Lazaris A Safioleas K Kontzoglou K January 2011 Medullary thyroid carcinoma The third most common thyroid cancer reviewed Oncol Lett 2 1 49 53 doi 10 3892 ol 2010 223 PMC 3412473 PMID 22870127 Dionigi G Bianchi V Rovera F et al 2007 Medullary thyroid carcinoma surgical treatment advances Expert Rev Anticancer Ther 7 6 877 85 doi 10 1586 14737140 7 6 877 PMID 17555398 S2CID 37519975 a b c Goldman L 2011 Goldman s Cecil Medicine 24th ed Philadelphia Elsevier Saunders pp e76 ISBN 978 1437727883 Fragu P 2007 Calcitonin s fantastic voyage from hormone to marker of a genetic disorder Gesnerus 64 1 2 69 92 doi 10 1163 22977953 0640102004 PMID 17982960 a b National Cancer Institute gt Medullary Thyroid Cancer Last Modified 12 22 2010 a b c Verbeek HH de Groot JW Sluiter WJ Muller Kobold AC van den Heuvel ER Plukker JT Links TP et al Cochrane Metabolic and Endocrine Disorders Group March 2020 Calcitonin testing for detection of medullary thyroid cancer in people with thyroid nodules The Cochrane Database of Systematic Reviews 2020 3 CD010159 doi 10 1002 14651858 CD010159 pub2 PMC 7075519 PMID 32176812 Schlumberger M Carlomagno F Baudin E Bidart JM Santoro M 2008 New therapeutic approaches to treat medullary thyroid carcinoma Nat Clin Pract Endocrinol Metab 4 1 22 32 doi 10 1038 ncpendmet0717 PMID 18084343 S2CID 25818628 Niederle B Sebag F Brauckhoff M 2013 Timing and extent of thyroid surgery for gene carriers of hereditary C cell disease a consensus statement of the European Society of Endocrine Surgeons ESES Langenbecks Arch Surg a b Thyroid Carcinoma PDF NCCN guidelines National Comprehensive Cancer Network Archived from the original PDF on 25 September 2006 Brierley J Tsang R Simpson WJ Gospodarowicz M Sutcliffe S Panzarella T 1996 Medullary thyroid cancer analyses of survival and prognostic factors and the role of radiation therapy in local control Thyroid 6 4 305 10 doi 10 1089 thy 1996 6 305 PMID 8875751 Quayle FJ Moley JF 2005 Medullary thyroid carcinoma including MEN 2A and MEN 2B syndromes J Surg Oncol 89 3 122 9 doi 10 1002 jso 20184 PMID 15719378 S2CID 31436486 American Thyroid Association Thyroid Clinical Trials Archived from the original on 2007 12 12 Retrieved 2007 12 21 FDA approves new treatment for rare form of thyroid cancer Food and Drug Administration Retrieved 7 April 2011 FDA approves Cometriq to treat rare type of thyroid cancer Food and Drug Administration Retrieved 29 November 2012 a b Numbers from National Cancer Database in the US from Page 10 in F Grunwald Biersack H J Grںunwald F 2005 Thyroid cancer Berlin Springer ISBN 978 3 540 22309 2 Barbet J Campion L Kraeber Bodere F Chatal JF November 2005 Prognostic impact of serum calcitonin and carcinoembryonic antigen doubling times in patients with medullary thyroid carcinoma The Journal of Clinical Endocrinology and Metabolism 90 11 6077 6084 doi 10 1210 jc 2005 0044 PMID 16091497 cancer org gt Thyroid Cancer Archived October 18 2013 at the Wayback Machine By the American Cancer Society In turn citing AJCC Cancer Staging Manual 7th ed a b Barbet J Campion L Kraeber Bodere F Chatal JF 2005 Prognostic impact of serum calcitonin and carcinoembryonic antigen doubling times in patients with medullary thyroid carcinoma J Clin Endocrinol Metab 90 11 6077 84 doi 10 1210 jc 2005 0044 PMID 16091497 ASCO Self Evaluation Program SEP American Society of Clinical Oncology ASCO External links edit Retrieved from https en wikipedia org w index php title Medullary thyroid cancer amp oldid 1182203466, wikipedia, wiki, book, books, library,

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