1. Diagnosis and dynamic assessment of persistent/recurrent and metastatic differentiated thyroid cancer (prmDTC)
Differentiated thyroid cancer (DTC), including papillary, follicular and Hürthle cell types, accounts for nearly 95% of all thyroid carcinomas. The concept of DTC recurrence or persistence after surgery is still difficult to define due to its indolent nature. The recurrent or persistent tumors in this guideline refer to new lesions or residual tumors found during the follow-up after initial treatments.
1.1 Basic principles of diagnosis
The role of multidisciplinary team (MDT) should be emphasized during the diagnosis of prmDTC. A task force of specialists with complementary expertise (endocrinology, surgery, nuclear medicine, radiology, pathology, oncology, molecular diagnostics, and epidemiology) should be included in the MDT management of prmDTC. The diagnosis or further managements of prmDTC which may include surgical managment, radioiodine-131 (131I) therapy, thyroid stimulating hormone (TSH) suppressive therapy, as well as molecular targeted therapy (or being enrolled in certain clinical trial) or radiation therapy, etc., should be tailored according to comprehensive consideration of MDT.
1.2 Diagnostic methods
Laboratory tests, imaging studies and pathological examinations are recommended in the diagnosis of prmDTC (Table 1).
1.
Diagnostic methods of prmDTC
| Methods | Level I recommendation | Level II recommendation |
|
a, Thyroglobulin (Tg) monitoring facilitates postoperative assessment and risk stratification. Low serum Tg level has a high negative predictive value in the absence of thyroglobulin antibody (TgAb) interference after initial treatment (1). Thyroglobulinemia out of proportion to what is seen on 131I-whole body scan (WBS) indicates the presence of distant metastasis (1-3). Tg also holds value in predicting the response or resistance to 131I therapy (4,5).
b, Simultaneous monitoring of Tg and TgAb levels is needed. The presence of TgAb will falsely lower serum Tg determinations in immunometric assays, and in this clinical setting, the serial monitoring of TgAb level may serve as a surrogate prognostic marker (6,7). c, Ultrasound (US) is considered the first-line imaging study for assessing locoregional lesions of persistent/recurrent and metastatic differentiated thyroid cancer (prmDTC), and experienced radiologists may enhance the diagnostic credibility in the management of such patients (1,8-11). d, The assessment of cervical ultrasonography includes cervical lymph nodes, thyroid beds, soft tissue, blood vessels, trachea and esophagus. Sonographic features of prmDTC are as follows (Figure 1). e, Frequently, it is not easy to distinguish thyroid bed recurrence from benign nodules. Interpretation of neck US should take into account clinical and biological data. f, Cross-sectional imaging studies, computed tomography (CT) or magnetic resonance imaging (MRI) with intravenous (IV) contrast, are recommended for suspicious prmDTC (12,13). g, 131I-WBS and single photon emission computed tomography (SPECT)/CT can be used to locate the iodine-avid foci, which is helpful in tailoring the subsequent 131I therapy (14,15). h, CT is routinely recommended for assessing patients with pulmonary metastases, 131I-WBS may play a complementary role in some patients with micrometastatic lesions which may be missed by chest CT (16,17). i, MRI is routinely recommended for assessing cerebral metastases (1). j, Bone scan is recommended for assessing suspicious bone metastases (18). k, 18F-fluorodeoxyglucose (18F-FDG) PET/CT is recommended in patients with elevated Tg (generally >10 ng/mL) or TgAb, especially in patients with non-radioiodine-avid foci ( 1,19-22). It may also be considered as a part of initial staging in poorly or invasive DTC and serve as a prognostic tool in prmDTC, especially in predicting those who are unlikely to benefit from 131I therapy (1). l, The gross examination should include the following: specimen type, tumor location, tumor size, gross morphology, relationship between the tumor and adjacent tissue structures, number of lymph nodes detected, size, and group. m, Microscopic examination should include the following: morphological variants, tumor size, dissemination, invasion range, resection margin, vascular invasion, nerve invasion, lymph node metastasis and total number, and TNM staging. For cases with morphological PTC, if possible, the possible histologic subtypes that may indicate poor prognosis, such as tall cell variant, columnar cell variant, diffuse sclerosing variant and hobnail variant, should be further reported (23). n, Commonly used immunohistochemical markers for determining the origin include CK, Tg, TTF-1, TTF-2, PAX-8, Syn, CgA, Calcitonin and CEA (24). Commonly used immunohistochemical markers for distingushing malignancy from benign lesion include galectin-3, HBME-1, CK19, CD56, E-cadherin, p27, cyclinD1, p53, Ki-67 index, etc. (24). o, Common molecular markers used to indicate malignancy or benign lesion include BRAFV600E, NRAS 61 codon, HRAS 61 codon and KRAS 12/13 codon mutations, RET/PTC and PAX8/PPARγ rearrangements, etc. (25). | ||
| Laboratory diagnosis | Serum Tga and TgAbb (2A) | Tg washout determination (2A) |
| Imaging diagnosis | Various image detections are as follows: | |
| Suspected local lesions | Neck ultrasoundc−e (2A), contrast CT or contrast MRIf (2A) | Ultrasound-guided fine needle aspiration cytology (2A), 131I-WBS + SPECT/CTg (2A),
18F-FDG PET/CT (2A) |
| Suspected distant metastasis | CTh (2A), 131I-WBS + SPECT/CT (2A), MRIi (suspected nervous system involvement) (2A), bone scanj (suspected bone involvement) (2A) | MRI (when organs other than the nervous system are involved) (2A), 18F-FDG PET/CTk (2A) |
| Pathological diagnosis | ||
| Previous pathology results | Confirmation of previous primary lesions | Review previous tissue specimens |
| Present pathology results | General inspectionl, microscopic examinationm of biopsy specimens | Immunohistochemistryn, molecular pathologyo (2A) |
1.3 Ongoing assessment of response to therapy (Table 2)
2.
Stratification of ongoing assessment of response to therapy
| Stratification | Definition (serology and imaging meet simultaneously) | Level I recommendation | |||
| Serology | Imaging | ||||
| Tg, thyroglobulin; TgAb, thyroglobulin antibody; TSH, thyroid stimulating hormone; FDG, fluorodeoxyglucose.
a, The risk of recurrence ranged from 1% to 4% over 5−10 years among ER patients. b, 15%−20% of IDR patients are reclassified as persistent/recurrent disease over approximately 10 years. c, 8%−17% of BIR patients developing structurally identifiable disease over 5−10 years. d, Death from disease was seen in 11% of patients with a loco-SIR and in 57% of patients with distant SIR. | |||||
| Excellent responsea (ER) | Suppressive Tg <0.2 ng/mL or stimulated Tg <1 ng/mL | Negative | Decrease of the intensity and frequency of follow-up and the degree of TSH suppression (1A) | ||
| Indeterminate responseb (IDR) | Non-stimulated Tg detectable, but less than 1 ng/mL. Stimulated Tg detectable, but less than 10 ng/mL. Or Tg antibodies stable or declining in the absence of structural or functional disease | Non-specific findings on imaging studies. Or faint uptake in thyroid bed on RAI scanning | Continuing observation with appropriate serial imaging of the nonspecific lesions and serum Tg monitoring. Nonspecific findings that become suspicious over time can be further evaluated with additional imaging or biopsy (1A) | ||
| Biochemical incomplete responsec (BIR) | Suppressed Tg >1 ng/mL, Stimulated Tg >10 ng/mL.
Or rising TgAb levels |
Negative | Those with stable or decreasing serum Tg levels may continue TSH suppression therapy and follow-up; patients with elevated serum Tg or TgAb should prompt additional investigations and potentially additional therapies (1A) | ||
| Structural incomplete responsed (SIR) | Serum Tg or TgAb at any level | Structural or functional evidence of disease | Additional treatments or ongoing observation depending on multiple clinicopathologic factors including the size, location, rate of growth, RAI avidity, 18FDG avidity, and specific pathology of the structural lesions (1A) | ||
As the risk of recurrence and cancer-related death in prmDTC may change over time, life long follow-up and periodical surveillance including laboratory and imaging evaluation are needed. Ongoing assessment of response to therapy should be used to guide the long-term surveillance and therapeutic management decision. In this guideline, we adopted the system of response to therapy which was put forward by 2015 American Thyroid Association Management Guidelines for Adult Patients with Thyroid Nodules and Differentiated Thyroid Cancer.
Multiple factors including clinical, biochemical, imaging (structural and functional) and cytopathology findings were taken into comprehensive consideration in this response system to assess the individual response to therapy during follow-up. It has been verified as an objective ongoing evaluation system to reflect the clinical outcomes from both the risk of recurrence and mortality (1). Four categories including excellent response (ER), indeterminate response (IDR), biochemical incomplete response (BIR) and structural incomplete response (SIR) are used to describe clinical outcomes at any time after initial treatment (1).
References
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2. Multidisciplinary treatment of prmDTC
2.1 Basic principles of treatment
Treatment options for prmDTCs usually include surgical resection, 131I therapy of lesions that can uptake 131I, external beam radiation therapy, active follow-up under L-T4 suppression therapy and other options (e.g., targeted medicines, radiofrequency or ethanol ablation). Among them, surgery should be the first choice for resectable lesions with surgical indications.
2.2 Surgical management
PrmDTCs are commonly seen in clinical practice, approximately 95% of which occur in the neck (1). Since the difficulty and risk of reoperation increase significantly, the risks and benefits of surgery must always be balanced when selecting reoperation. Surgery should be performed by experienced specialists, and frequently even under multidisciplinary collaboration.
2.2.1 Preoperative clinical assessment
Preoperative clinical assessment includes the review of previous treatments, current status of the disease and vital organ function, which are the basis for the decision regarding intervention and extent of revision surgery. Structural lesions are required as a target for a surgical revision approach, therefore, imaging evaluation is of the utmost importance to surgeons to identify and localize the structural lesions (Table 3).
3.
Recommendations of preoperative clinical assessment
| Evaluation
contenta |
Level I
recommendation |
Level II
recommendation |
Level III
recommendation |
| PTH, parathyroid hormone; CT, computed tomography; MRI, magnetic resonance imaging; WBS, whole body scan; SPECT, single photon emission computed tomography; FDG, fluorodeoxyglucose.
a, Thyroglobulin (Tg), Tg antibody (TgAb) and imaging examinations can be used to evaluate the current state of disease. Neck ultrasonography is the most important technique to detect structural lesions (2,3). | |||
| Clinical data | Preoperative and pathological record review Complications of previous surgery, such as hematoma, infection, etc.
Physical exam, esp. special signs for recurrent metastases. |
— | — |
| Laboratory tests | Serum Tg, TgAb, see 1.2 Diagnostic methods (2A) Parathyroid function evaluation: serum calcium and PTH levels | — | — |
| Routine examination | Neck ultrasound (2A)
Contrast neck CT or MRI, chest CT, etc. See 1.2 Diagnostic methods (2A) Assessment of vocal cords movement and recurrent laryngeal nerve function assessment Laryngoscopy, when trachea involvement is suspected. Esophagoscopy, when esophagus involvement is suspected. |
CT angiogram or MR angiogram (MRA) when suspected of vascular involvement
131I-WBS + SPECT/CT and 18F-FDG PET/CT if necessary, see 1.2 Diagnostic methods (2A) |
— |
2.2.2 Principles of surgical treatment for prmDTC
The timing and extent of surgery are the most important issues which should be considered when the surgical management of prmDTC is decided. In general, the goal of revision surgery should be to try to cure or control the disease, improve survival, and preserve the function of the vital organs as far as possible (Table 4).
4.
Recommendations of surgical treatment principles
| Lesions | Level I
recommendation |
Level II
recommendation |
Level III
recommendation |
| Cervical lesions without invasion to surrounding vital structuresa | |||
| Central
compartment |
Preservation in situ or autotransplantation of parathyroid glandsb (2A) | Active follow-up: lesion <8 mm in the smallest dimension (2A)
Consider reoperation: lesion ≥8 mm in the smallest dimension (2A) Preoperative FNA (2A) Completion of thyroidectomy and standardized central compartment neck dissection (2A) Intraoperative Neuromonitoring (IONM) of the recurrent laryngeal nerveb (2A) |
Ipsilateral central neck dissection in patient without bilateral central compartment involvement (2B) |
| Lateral
compartment |
— | Active follow-up: lesion <10 mm in the smallest dimension (2A)
Consider reoperation: lesion ≥10 mm in the smallest dimension (2A) Preoperative FNA (2A) Therapeutic modified radical neck dissection and preservation of vital structures for previously undissected compartments (2A) Limited neck dissection (generally includes levels II, III, IV, or 1-2 levels of them) for previously managed compartments, due to extensive scar and unclear anatomy (2A) |
— |
| Cervical lesions with invasion to surrounding vital structuresc | |||
| Recurrent
laryngeal nerve involvementd |
Shave the tumor off as much as possible and preserve the nerve in patient without vocal cord paralysis (2A)
Remove lesions and the affected nerve in patient with preoperative vocal cord paralysis or intraoperative finding of complete tumor encapsulation of the nerve (2A) |
Nerve reinnervation simultaneously at surgery after resection or injury of the nerve, if feasible (2A) Second-look operation with nerve repair for postoperative identification of recurrent laryngeal nerve injury (2A) | — |
| Airway/digestive
tract (larynx trachea/ esophagus) involvemente |
— | Consider shaving tumor in patient with no intraluminal tumor invasion (2A)
Resection of the lesion and involved organs in patient with intraluminal tumor invasion; If feasible, simultaneous airway/digestive tract repair and reconstruction, otherwise, tracheostomy (2A) Palliative surgery, such as tracheostomy or gastrostomy, in patients having asphyxiation or hemoptysis symptoms with unresectable lesions (2A) |
— |
| Table 4 (continued) | |||
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2.3 131I therapy
131I therapy is one of the important adjuvant postoperative treatment modalities for prmDTC patients. It can reduce the risks of tumor recurrence, metastasis and death in high risk population (1,2), and significantly improve the 5- and 10-year survival for high-risk DTC patients with iodine-avid lesions (3-9).
131I therapy is recommended in patients with iodine-avid prmDTC lesions, and should be repeated at an interval of 6−12 months as long as the lesions continue to concentrate radioiodine and respond clinically. In addition, cumulative radioiodine activities, balance between benefits and risks, and patient preferences, are relevant to131I therapy decision-making. Patients with TSH stimulation and iodine preparation, whose lesions no longer concentrate 131I or respond to 131I therapy, are identified as radioactive iodine refractory DTC (RAIR-DTC) in four basic ways: 1) the malignant metastatic lesion does not ever concentrate RAI (no uptake outside the thyroid bed at the first therapeutic WBS); 2) the tumor tissue loses the ability to concentrate RAI after previous evidence of RAI-avid disease (in the absence of stable iodine contamination); 3) RAI is concentrated in some lesions but not in others; and 4) disease progresses despite significant concentration of RAI (10).
2.3.1 Clinical assessment before 131I therapy
Clinical information, as well as the status exactly before 131I therapy should be considered for tailoring the management of prmDTC (Table 5). Further surgical consultation should be advised if a patient has lesions which might be amenable to surgery. While in terms of the clinical information, evaluation of the response to previous therapeutics is critical for subsequent 131I therapy of prmDTC, for instance, a previous 131I unresponsive patient would be unlikely to benefit from another repeated 131I therapy.
5.
Recommendations of pretherapeutic evaluation for initial/further 131I therapy in prmDTC patients
| Evaluation content | Level I
recommendation |
Level II
recommendation |
Level III
recommendation |
| prmDTC, persistent/recurrent and metastaticdifferentiated thyroid cancer; WBS, whole body scan; CT, computed tomography; MRI, magnetic resonance imaging; FDG, fluorodeoxyglucose; PET, positron emission tomography.
a, Serum TSH should be >30 mIU/L through L-T 4 withdrawl before 131I therapy (11,12). Currently, thyrogen is not approved by CFDA. b, Diagnostic WBS (Dx-WBS) can be used for identifying radioiodine-avid lesions, tailoring dosage of 131I, and predicting the efficacy of 131I therapy (1). c, BRAFV600E mutation is the most common oncogenic mutation and related to aggressive disease, recurrence and mortality. BRAFV600E mutation in isolation or in combination with TERT mutation appears to be associated with more aggressive tumor behavior, and more likely to be refractory to 131I therapy (1,13,14). | |||
| Clinical information | Evaluate the response and adverse events to previous therapeutics, including surgery, 131I therapy, and TSH suppression, etc.a
Physical examination |
— | — |
| Laboratory tests | Thyroid hormones, TSH (2A)
Tg, TgAb (2A) Complete blood count, hepatic and renal function test |
Serum/Urine iodine measurement | — |
| Routine examination | Electrocardiogram (ECG) | Cardiac ultrasound or dynamic ECG | — |
| Imaging examination | Diagnostic 131I WBSb (2A)
Cervical ultrasonography (2A) CT (2A) |
Bone scan (2A)
MRI (2A) 18F-FDG PET/CT (2A) |
— |
| Pathological examination | — | BRAFV600E mutation detectionc (2A) | — |
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Professional Committee of Thyroid Cancer, Chinese Society of Clinical Oncology. Consensus on diagnosis and treatment of recurrent and metastatic differentiated thyroid cancer. Zhongguo Ai Zheng Za Zhi (in Chinese) 2015;25:481-96.
Yang K, Wang H, Liang Z, et al. BRAFV600E mutation associated with non-radioiodine-avid status in distant metastatic papillary thyroid carcinoma. Clin Nucl Med 2014;39:675-9.
Yang X, Li J, Li X, et al. TERT promoter mutation predicts radioiodine-refractory character in distant metastatic differentiated thyroid cancer. J Nucl Med 2017;58:258-65.
2.3.2 Management of 131I therapy for prmDTC
Indications and dose determination of 131I therapy for prmDTC are addressed in terms of the sites of metastases (Table 6).
6.
Recommendations for 131I administration in prmDTC patients
| Items | Recommendation | ||
| Level I | Level II | Level III | |
| Indications of 131I therapy for prmDTC | |||
| Local lesions | — | 131I therapy (iodine-avid lesions)a (2A) | — |
| Lung metastases | 131I therapy (iodine-avid lesions)b (1B) | — | — |
| Bone metastases | — | 131I therapy (iodine-avid lesions)c (2A) | — |
| Brain metastases | — | — | 131I therapy (iodine-avid lesions)d (2B) |
| Tg(+)131I(−) | — | — | Empirical 131I therapye |
| Preparation for 131I therapy | |||
| TSH >30 mIU/L | Levothyroxine (L-T4)
withdrawal for at least 2−4 weeks (2A) |
Liothyronine (L-T3) may be substituted for L-T4 for at least
4 weeks, and then should be withdrawn for at least 2 weeks (2A) rhTSHf (2A) |
— |
| Low iodine diet | Low iodine diet for at least 2 weeksg (2A) | — | — |
| Table 6 (continued) | |||
References
Chinese Society of Nuclear Medicine. Clinical guidelines for 131I therapy of differentiated thyroid cancer. Zhonghua He Yi Xue Yu Fen Zi Ying Xiang Za Zhi (in Chinese) 2014;34:264-78.
Haugen, BR, Alexander EK, Bible KC, et al. 2015 American thyroid association management guidelines for adult patients with thyroid nodules and differentiated thyroid cancer: The American thyroid association guidelines task force on thyroid nodules and differentiated thyroid cancer. Thyroid 2016;26:1-133.
Piccardo A, Puntoni M, Bottoni G et al. Differentiated Thyroid Cancer lymph-node relapse. Role of adjuvant radioactive iodine therapy after lymphadenectomy. Eur J Nucl Med Mol Imaging 2017;44:926-34.
Song HJ, Qiu ZL, Shen CT, et al. Pulmonary metastases in differentiated thyroid cancer: efficacy of radioiodine therapy and prognostic factors. Eur J Endocrinol 2015;173:399-408.
Ronga G, Filesi M, Montesano T, et al. Lung metastases from differentiated thyroid carcinoma. A 40 years’ experience. Q J Nucl Med Mol Imaging 2014;48:12-9.
Schlumberger M, Challeton C, De Vathaire F, et al. Radioactive iodine treatment and external radiotherapy for lung and bone metastases from thyroid carcinoma. J Nucl Med 1996;37:598-605.
Ilgan S, Karacalioglu AO, Pabuscu Y, et al. Iodine-131 treatment and high-resolution CT: results in patients with lung metastases from differentiated thyroid carcinoma. Eur J Nucl Med Mol Imaging 2004;31:825-30.
Hod N, Hagag P, Baumer M, et al. Differentiated thyroid carcinoma in children and young adults: evaluation of response to treatment. Clin Nucl Med 2005;30:387-90.
Fatourechi V, Hay ID, Javedan H, et al. Lack of impact of radioiodine therapy in tg-positive, diagnostic whole-body scan-negative patients with follicular cell-derived thyroid cancer. J Clin Endocrinol Metab 2002;87:1521-6.
Koh JM, Kim ES, Ryu JS, et al. Effects of therapeutic doses of 131I in thyroid papillary carcinoma patients with elevated thyroglobulin level and negative 131I whole-body scan: comparative study. Clin Endocrinol (Oxf) 2003;58:421-7.
Bernier MO, Leenhardt L, Hoang C, et al. Survival and therapeutic modalities in patients with bone metastases of differentiated thyroid carcinomas. J Clin Endocrinol Metab 2001;86:1568-73.
Professional Committee of Thyroid Cancer, Chinese Society of Clinical Oncology. Consensus on diagnosis and treatment of recurrent and metastatic differentiated thyroid cancer. Zhongguo Ai Zheng Za Zhi (in Chinese) 2015;25:481-96.
Molenaar RJ, Sidana S, Radivoyevitch T, et al. Risk of hematologic malignancies after radioiodine treatment of well-differentiated thyroid cancer. J Clin Oncol 2018;36:1831-9.
National Comprehensive Cancer Network. NCCN Clinical Practice Guidelines in Oncology (NCCN Guidelines®): Thyroid Carcinoma Version 2. 2017.
2.4 TSH suppression therapy
2.4.1 Strategy for TSH suppression therapy
For prmDTC that expresses TSH receptor, TSH suppression therapy is important in postoperative management of differentiated thyroid cancer. It has been realized the optimal degree of TSH suppression varies. An individually tailored approach to deciding TSH targets in prmDTC patients considering risk of side effects has been raised (Table 7).
7.
Strategy for TSH suppression therapy
| Treatment period | Level I recommendation | Level II recommendation |
| ER, excellent response; IDR, indeterminate response; BIR, biochemical incomplete response; SIR, structural incomplete response.
a, If the tumor is poorly differentiated and no longer expresses thyroid stimulating hormone (TSH) receptor, only thyroid hormone replacement is needed (1,2). b, The initial treatment period refers to within one year after the persistent/recurrent and metastatic differentiated thyroid cancer (prmDTC) being treated with surgery and/or radioactive iodine (3,4). c, The long-term follow-up period refers to one year after the prmDTC being treated with surgery and/or radioactive iodine (3,4). TSH suppression goals may not be uniform and should be adjusted according to results of surveillance (5-8). | ||
| Whole-coursea | Applicable patients: prmDTC expresses TSH receptor (category 1A)
First-line medication: oral L-T4 agents (category 1A) Starting L-T4 dose: based on patient's age and co-existing diseases Final L-T4 dose: titrated according to patient’s TSH goal and results of monitoring (category 1A) Check TSH every 4−6 weeks during the L-T4 dose adjustment (category 1A) |
—
Extend intervals of TSH monitor to 3−6 months once TSH reaches the goal (category 2A) |
| Initial periodb | TSH target based on risks of TSH suppression therapy (category 1A)
-Low risk: <0.1 mU/L (category 2A) -High risk: If tolerated, <0.1 mU/L to lower normal limit (category 2A) |
— |
| Long-term follow-up periodc | TSH target based on dynamic assessments
(category 2A) |
-ER: lower normal limit to 2.0 mU/L (category 2A)
-IDR: around the lower normal limit of TSH (category 2A) -BIR: 0.1 mU/L to lower normal limit; If risk of side effects of TSH suppression is low, <0.1 mU/L (category 2A) -SIR: If tolerated, <0.1 mU/L (category 2A) |
References
Biondi B, Filetti S, Schlumberger M. Thyroid hormone therapy and thyroid cancer: a reassessment. Nat Clin Pract Endocrinol Metab 2005;1:32-40.
Biondi B, Wartofsky L. Treatment with thyroid hormone. Endocr Rev 2014;35:433-512.
Chinese Society of Endocrinology, Chinese Society of General Surgery Endocrinology Group, China Anti-Cancer Association Head and Neck Tumor Professional Committee, et al. Guidelines on the Diagnosis and Treatment of Thyroid Nodules and Differentiated Thyroid Carcinomas. Zhonoghua Nei Fen Mi Dai Xie Za Zhi (in China) 2012;28:779-97.
Haugen, BR, Alexander EK, Bible KC, et al. 2015 American thyroid association management guidelines for adult patients with thyroid nodules and differentiated thyroid cancer: The American thyroid association guidelines task force on thyroid nodules and differentiated thyroid cancer. Thyroid 2016;26:1-133.
Diessl S, Holzberger B, Mäder U, et al. Impact of moderate vs stringent TSH suppression on survival in advanced differentiated thyroid carcinoma. Clin Endocrinol (Oxf) 2012;76:586-92.
Biondi B, Cooper DS. Benefits of thyrotropin suppression versus the risks of adverse effects in differentiated thyroid cancer. Thyroid 2010;20:135-46.
Carhill AA, Litofsky DR, Ross DS, et al. Long-term outcomes following therapy in differentiated thyroid carcinoma: NTCTCS registry analysis 1987-2012. J Clin Endocrinol Metab 2015;100:3270-9.
Momesso DP, Tuttle RM. Update on differentiated thyroid cancer staging. Endocrinol Metab Clin North Am 2014;43:401-21.
2.4.2 Management of adverse effects of TSH suppression therapy
When TSH has to be suppressed below the normal range (i.e. subclinical thyrotoxicosis) for a long period, especially below 0.1 mU/L, it may cause adverse effects (AEs) (Table 8).
8.
Management of adverse effects of TSH suppression therapy
| Adverse events (AE) | Level I recommendation | Level II recommendation |
|
a,When thyroid stimulating hormone (TSH) has to be suppressed below the normal range (i.e. subclinical thyrotoxicosis) for a long period, especially below 0.1 mU/L, it may cause AE, mainly involving cardiovascular system, as well as skeletal system in postmenopausal women (1-5).
b, Patients with underlying heart diseases or high risk of cardiovascular events should be given appropriate treatments by specialists, and their TSH targets should be adjusted accordingly (6-9). c, Particular attention is warranted for female patients after menopause (10). | ||
| All AEa | Set individualized TSH targets, monitor AEs and adjust L-T4 doses in a timely manner (1A) | — |
| Cardiovascular AEb | Baseline cardiovascular assessment (2A), β blockers (2A) | — |
| Skeletal system AEc | Baseline skeletal assessment (2A), primary prevention of osteoporosis (OP); anti-OP treatment (2A) | — |
References
Cooper DS, Biondi B. Subclinical thyroid disease. Lancet 2012;379:1142-54.
Klein Hesselink EN, Klein Hesselink MS, de Bock GH, et al. Long-term cardiovascular mortality in patients with differentiated thyroid carcinoma: an observational study. J Clin Oncol 2013;31:4046-53.
Flynn RW, Bonellie SR, Jung RT, et al. Serum thyroid-stimulating hormone concentration and morbidity from cardiovascular disease and fractures in patients on long-term thyroxine therapy. J Clin Endocrinol Metab 2010;95:186-93.
Haugen BR, Alexander EK, Bible KC, et al. 2015 American Thyroid Association management guidelines for adult patients with thyroid nodules and differentiated thyroid dancer: the American Thyroid Association guidelines task force on thyroid nodules and differentiated thyroid cancer. Thyroid 2016;26:1-133.
Rieben C, Segna D, da Costa BR, et al. Subclinical thyroid dysfunction and the risk of cognitive decline: a meta-analysis of prospective cohort studies. J Clin Endocrinol Metab 2016;101:4945-54.
Carié A, Andersen SL, Boelaert K, et al. Management of endocrine disease: Subclinical thyrotoxicosis: prevalence, causes and choice of therapy. Eur J Endocrinol 2017;176:325-37.
Jabbar A, Pingitore A, Pearce SH, et al. Thyroid hormones and cardiovascular disease. Nat Rev Cardiol 2017;14:39-55.
Ross DS, Burch HB, Cooper DS, et al. 2016 American Thyroid Association Guidelines for Diagnosis and Management of Hyperthyroidism and Other Causes of Thyrotoxicosis. Thyroid 2016;26:1343-421.
Chinese Society of Endocrinology, Chinese Society of General Surgery Endocrinology Group, China Anti-Cancer Association Head and Neck Tumor Professional Committee, et al. Guidelines on the Diagnosis and Treatment of Thyroid Nodules and Differentiated Thyroid Carcinomas. Zhonoghua Nei Fen Mi Dai Xie Za Zhi (in Chinese) 2012;28:779-97.
Chinese Society of Bone and Mineral Research. Diagnosis and treatment guidelines for primary osteoporosis (2017). Zhonghua Gu Zhi Shu Song He Gu Kuang Yan Ji Bing Za Zhi (in Chinese) 2017;10:413-43.
2.5 External beam radiation therapy
External beam radiation therapy (EBRT) is an effictive and safe local therapy with benefit to local control and palliative care for prmDTC. EBRT, stereotactic radiation therapy (SBRT) and other local therapies can be used for symptomatic, weight-bearing, key site metastasis, and oligo-metastasis (Table 9).
9.
Recommendation of external beam radiation therapy for prmDTC
| Lesions | Level I recommendation | Level II recommendation | Level III recommendation |
|
a, External beam radiation therapy (EBRT) and stereotactic radiation therapy (SBRT) can be considered for persistent/recurrent and metastatic differentiated thyroid cancer (prmDTC), such as local recurrence and distant metastasis, especially for non-iodine-avid disease or RAI-rafractory throid cancer (1,2).
b, The optimal target volume and dose for EBRT are still controversial (3,4). Conventional fractionation radiotherapy dose is: 1) Gross target volume (GTV, mainly including recurrent or residual tumor regions, metastase): 60−70 Gy; and 2) Clinical target volume (CTV, mainly including subclinical area): 50−60 Gy (5). Precise radiotherapy technologies, such as intensity-modulated radiotherapy (IMRT) and image guided radiotherapy (IGRT), are safe, effective, and less morbid (6,7). c, In the case of DTC lung metastases, EBRT or SBRT mainly applies to: 1) Single or oligo-metastasis (the definition of oligo-metastasis is not uniformly standardized, and it is generally considered that the number of metastases is ≤3−4); and 2) Lung metastases that do not intake iodine (8). d, EBRT or SBRT can be mainly considered for symptomatic skeletal metastases or those that are asymptomatic in weight-bearing sites. The main role is to relieve the pain symptoms, reduce the risk of pathological bone events, and improve the quality of life (9,10). e, EBRT or SBRT is one of the main treatments for brain metastases regardless of the number and size of lesions, or the iodine intake status. Once brain metastases are diagnosed, disease-specific mortality is very high (67%), with median survival of 12.4 months. Survival can be significantly improved by neurosurgical resection. With the development of radiotherapy techniques, SBRT can achieve similar results to neurosurgery (11-13). | |||
| Local recurrent lesions | — | EBRT (unresectable local recurrent lesions)a,b (2A) | — |
| Metastatic lesions | — | — | — |
| Lung metastases | — | EBRT/SBRT (single or oligo-metastasis)c (2A) | EBRT/SBRT (selective for multiple metastases) (2B) |
| Bone metastases | — | EBRT/SBRT (symptomatic or weight bearing bones)d (2A) | — |
| Brain metastases | EBRT/SBRT (single or
oligo-metastasis)e (2A) |
EBRT/SBRT (multiple metastases) (2B) | — |
| Other metastases | — | EBRT/SBRT (non-iodine-avid disease, palliative relief of local symptoms) (2B) | — |
References
Hamilton SN, Tran E, Berthelet E, et al. The role of external beam radiation therapy in well-differentiated thyroid cancer. Expert Rev Anticancer Ther 2017;17:905-10.
Mikalsen LTG, Arnesen MR, Bogsrud TV, et al. Combining radioiodine and external beam radiation therapy: the potential of integrated treatment planning for differentiated thyroid cancer. Acta Oncol 2017;56:894-7.
Vulpe H, Kwan JYY, McNiven A, et al. Patterns of failure in anaplastic and differentiated thyroid carcinoma treated with intensity-modulated radiotherapy. Curr Oncol 2017;24:e226-32.
Kim TH, Chung KW, Lee YJ, et al. The effect of external beam radiotherapy volume on locoregional control in patients with locoregionally advanced or recurrent nonanaplastic thyroid cancer. Radiat Oncol 2010;5:69.
Mangoni M, Gobitti C, Autorino R, et al. External beam radiotherapy in thyroid carcinoma: clinical review and recommendations of the AIRO “Radioterapia Metabolica” Group. Tumori 2017;103:114-23.
Lee EK, Lee YJ, Jung YS, et al. Postoperative simultaneous integrated boost-intensity modulated radiation therapy for patients with locoregionally advanced papillary thyroid carcinoma: preliminary results of a phase II trial and propensity score analysis. J Clin Endocrinol Metab 2015;100:1009-17.
Tam S, Amit M, Boonsripitayanon M, et al. Adjuvant external beam radiotherapy in locally advanced differentiated thyroid cancer. JAMA Otolaryngol Head Neck Surg 2017;143:1244-51.
Rieber J, Streblow J, Uhlmann L, et al. Stereotactic body radiotherapy (SBRT) for medically inoperable lung metastases-A pooled analysis of the German working group “stereotactic radiotherapy”. Lung Cancer 2016;97:51-8.
Lo SS, Lutz ST, Chang EL, et al. ACR Appropriateness Criteria (R) Spinal Bone Metastases. J Palliat Med 2013;16:9-19.
Lutz ST, Lo SS, Chang EL, et al. ACR Appropriateness Criteria(R) non-spine bone metastases. J Palliat Med 2012;15(5):521-6.
Linskey ME, Andrews DW, Asher AL, et al. The role of stereotactic radiosurgery in the management of patients with newly diagnosed brain metastases: a systematic review and evidence-based clinical practice guideline. J Neurooncol 2010;96:45-68.
Henriques de Figueiredo B, Godbert Y, Soubeyran I, et al. Brain metastases from thyroid carcinoma: a retrospective study of 21 patients. Thyroid 2014;24:270-6.
Lutz S, Balboni T, Jones J, et al. Palliative radiation therapy for bone metastases: Update of an ASTRO Evidence-Based Guideline. Pract Radiat Oncol 2017;7:4-12.
2.6 Systemic therapy
Close follow-up is recommended in patients identified as RAIR-DTC. The degree of disease progression should be factored into treatment decisions. Systemic therapy, including chemotherapy and molecular targeted therapy, should be considered in RAIR-DTC patients with rapidly progressive and/or symptomatic disease. Potential benefits and risks of systemic therapy should be thoroughly balanced in the candidates (Table 10, 11).
10.
Stratified recommendations for potential systemic therapy in RAI-refractory prmDTC patients
| Stratificationa | Level I
recommendation |
Level II
recommendation |
Level III
recommendation |
|
a, Patients with very indolent disease who are asymptomatic may not be appropriate for systemic therapy, and the follow-up strategy of every 3−6 months is recommended. Whereas patients with more rapidly progressive disease may benefit from systemic therapy (1,2).
b, The following points should be taken into consideration when patients are tentatively regarded as candidates for molecular targeted therapy (3-7): 1) The benefit of molecular targeted therapy may primarily yield the prolongation of progression-free survival (PFS) rather than overall survival (OS); 2) Molecular targeted drugs may induce adverse effects and result in low quality of life (QoL); and 3) Despite radioactive iodine refractory (RAIR), the disease may remain stable for several months to several years. c, Sorafenib is the first targeted drug applied in a completed randomized, double-blind, phase 3 trial for the treatment of locally advanced or metastatic RAIR-DTC (8). It was approved by China Food and Drug Administration (CFDA) in March 2017 for the treatment of progressive RAIR-DTC (9). Considering the balance of efficacy and side effects, 400 mg b.i.d. has been commonly utilized in most clinical trials (10-13); but the applications of low-dose sorafenib (200 mg b.i.d.) for treatment of RAIR-DTC could also achieve well efficacy with slight side effects, which may improve the compliance of patients and reduce medical costs (9,14). d, The indications of clinical trials in this entity may include: 1) Locally advanced or metastatic RAIR-DTC patients with disease progression determined by Response Evaluation Criteria In Solid Tumors (RECIST); and 2) Patients with BRAF, PPARγ or other tumor-related gene mutations which could be targeted by molecular drugs. e, Chemotherapy is only a palliative or experimental method for persistent/recurrent and metastatic differentiated thyroid cancer (prmDTC) with no response to other treatment. Adriamycin is the only chemotherapeutic drug approved by the US FDA (15,16). f, Molecular targeted therapy-induced adverse effects are common, and may lead to dose reduction and drug discontinuation. Common adverse effects reported include skin toxicity, hypertension, gastrointestinal toxicity, proteinuria, fatigue, thyroid-stimulating hormone inhibitory disorders, and impaired thyroid function. Before treatment, comprehensive assessment of certain risk factors that may increase the risk of adverse effects and necessary intervention to control concomitant diseases are recommended. For adverse effects during treatment, multidisciplinary consultation should be considered to protect important organs, improve the quality of life, and maximize the effects of targeted drugs. If the degree of adverse reactions is low and the function of important organs is well, the sustained targeted therapy is recommended to obtain the maximum curative effect and survival benefit from targeted drugs; if grade 3−4 adverse effects or the damage of important organs occur, the dose reduction or drug discontinuation should be promptly adopted until the weakening or disappearance of adverse effects, and then the therapy should restart from a lower dose. | |||
| Asymptomatic, stable or slow progression | Regular follow-up (2A) | Participation in clinical trialsd (2A) | — |
| Symptomatic or rapid progression | Sorafenibb,c (1) | Adriamycine (2A); Participation in clinical trials (2A) | — |
| Termination of targeted therapy | Tumor response evaluated to be progressive disease (PD) according to RECIST (1A)
Serious drug-related adverse reactions that cannot be tolerated for continued treatmentf (1A) |
Tg continues to rise or fail to decrease without disease remission according to RECIST (2A) | — |
11.
Efficacy of molecular targeted drugs for thyroid cancer therapeutics
| Medicines | Pathological type | Experimental design | Number of cases | ORR | Median PFS (month) | References |
| ORR, objective response rate; PFS, proression-free survival; RAIR-DTC, radioactive iodine refractory differentiated thyroid cancer; MTC, medullary thyroid carcinoma; RCT, randomized controlled clinical trial; PLC, placebo; SOR, sorafenib; LEN, lenvatinib; VAN, vandetanib; NR, not reported; NE, not evaluated.
a, The SELEC study showed that lenvatinib significantly prolonged PFS in RAIR-DTC compared with placebo (17). Lenvatinib mesylate has been approved by the European Commission for the treatment of invasive, locally advanced or metastatic DTCs. b, A single-arm prospective clinical trial had been conducted to evaluate the efficacy and safety of apatinib in the treatment of advanced RAIR-DTC, suggesting well tolerance with rapid-onset efficacy and high-rate of objective response in the first 8-week therapy (18). | ||||||
| Sorafenib | RAIR-DTC | Phase III
RCT vs. PLC |
207 SOR, 210 PLC | 12.2% vs. 0.5% | 10.8 vs. 5.8 | Lancet 2014; 384:319-28. |
| Lenvatiniba | RAIR-DTC | Phase III
RCT vs. PLC |
261 LEN, 131 PLC | 64.8% vs. 1.5% | 18.3 vs. 3.6 | New England journal of medicine 2015;372: 621-30. |
| Apatinibb | RAIR-DTC | Phase II | 10 | 90% | NR | Oncotarget 2017;8:42252-61. |
| Pazopanib | RAIR-DTC | Phase II | 37 | 49% | 11.7 | The Lancet Oncology 2010;11:962-72. |
| Sunitinib | RAIR-DTC | Phase II | 23 | 26% | 8 | European Journal of Endocrinology 2016;174:373-80. |
| RAIR-DTC/MTC | Phase II | 27 RAIR-DTC, 7 MTC | 31% | NR | Clinical cancer research 2010;16:5260-8. | |
| Axitinib | RAIR-DTC/MTC | Phase II | 45 RAIR-DTC, 11 MTC | 30% | 16.1 | Cancer 2014;120:2694-703. |
| RAIR-DTC/MTC | Phase II | 45 RAIR-DTC, 6 MTC | 35% | 15 | Cancer Chemotherapy and Pharmacology 2014;74:1261-70. | |
| Vandetanib | RAIR-DTC | Phase II
RCT vs. PLC |
72 VAN, 73 PLC | 8% vs. 5% | 11.1 vs. 5.9 | The Lancet Oncology 2012;13:897-905. |
| Cabozantinib | RAIR-DTC | Phase I | 15 | 53% | NE | Thyroid 2014;24:1508-14. |
References
Sabra MM, Dominguez JM, Grewal RK, et al. Clinical outcomes and molecular profile of differentiated thyroid cancers with radioiodine-avid distant metastases. J Clin Endocrinol Metab 2013;98:E829-36.
Schlumberger M, Brose M, Elisei R, et al. Definition and management of radioactive iodine-refractory differentiated thyroid cancer. Lancet Diabetes Endocrinol 2014;2:356-8.
Haugen, BR, Alexander EK, Bible KC, et al. 2015 American Thyroid Association Management Guidelines for Adult Patients with Thyroid Nodules and Differentiated Thyroid Cancer: The American Thyroid Association Guidelines Task Force on Thyroid Nodules and Differentiated Thyroid Cancer. Thyroid 2016;26:1-133.
National Comprehensive Cancer Network. NCCN Clinical Practice Guidelines in Oncology (NCCN Guidelines®): Thyroid Carcinoma Version 2. 2017.
Chinese Society of Endocrinology, Chinese Society of General Surgery Endocrinology Group, China Anti-Cancer Association Head and Neck Tumor Professional Committee, et al. Guidelines on the Diagnosis and Treatment of Thyroid Nodules and Differentiated Thyroid Carcinomas. Zhonoghua Nei Fen Mi Dai Xie Za Zhi (in Chinse) 2012;28:779-97.
Perros P, Boelaert K, Colley S, et al. Guidelines for the management of thyroid cancer. Clin Endocrinol (Oxf) 2014;81 Suppl 1:1-122.
Pacini F, Castagna MG, Brilli L, et al. Thyroid cancer: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up. Ann Oncol 2012 Suppl 7;23:110-9.
Brose MS, Nutting CM, Jarzab B, et al. Sorafenib in radioactive iodine-refractory, locally advanced or metastatic differentiated thyroid cancer: a randomized, double-blind, phase 3 trial. Lancet 2014;384:319-28.
Chen L, Shen Y, Luo Q, et al. Response to sorafenib at a low dose in patients with radioiodine-refractory pulmonary metastases from papillary thyroid carcinoma. Thyroid 2011;21:119-24.
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Kloos RT, Ringel MD, Knopp MV, et al. Phase II trial of sorafenib in metastatic thyroid cancer. J Clin Oncol 2009;27:1675-84.
Hoftijzer H, Heemstra KA, Morreau H, et al. Beneficial effects of sorafenib on tumor progression, but not on radioiodine uptake, in patients with differentiated thyroid carcinoma. Eur J Endocrinol 2009;161:923-31.
Cabanillas ME, Waguespack SG, Bronstein Y, et al. Treatment with tyrosine kinase inhibitors for patients with differentiated thyroid cancer: the M. D. Anderson experience. J Clin Endocrinol Metab 2010;95:2588-95.
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Schlumberger M, Tahara M, Wirth LJ, et al. Lenvatinib versus placebo in radioiodine-refractory thyroid cancer. N Engl J Med 2015;372:621-30.
Lin Y, Wang C, Gao W, et al. Overwhelming rapid metabolic and structural response to apatinib in radioiodine refractory differentiated thyroid cancer. Oncotarget 2017;8:42252-61.
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Working group members
Chair: Yansong Lin
Associate chair: Huiqiang Huang, Ye Guo, Libo Chen
Task force member (listed alphabetically by last name) (*, writing member)
Jiandong Bao Jiangsu Institute of Nuclear Medicine, Jiangsu Jiangyuan Hospital, Wuxi Institute of Thyroid Diseases
Ge Chen Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Libo Chen* Shanghai Jiao Tong University Affiliated Sixth People’s Hospital
Yali Cui Affiliated Tumor Hospital, Harbin Medical University
Yong Ding* Beijing People’s Liberation Army 307 Hospital
Haixia Guan* The First Hospital of China Medical University
Ye Guo* Shanghai East Hospital, Tongji University
Zairong Gao* Union Hospital, Tongji Medical College, Huazhong University of Science and Technology
Huiqiang Huang Affiliated Tumor Hospital, Sun Yat-sen University
Rui Huang* West China Hospital, Sichuan University
Tao Huang Union Hospital, Tongji Medical College, Huazhong University of Science and Technology
Xiaorong Hou* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Xiayun He* Cancer Hospital, Fudan University
Mei Li* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Shaohua Li Nanjing First Hospital
Xiaoyi Li* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Xuena Li The First Hospital of China Medical University
Yujun Li Affiliated Hospital of Qingdao University, Qingdao University
Zhiyong Liang* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Yukun Luo Chinese People’s Liberation Army General Hospital
Yansong Lin* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Jing Lyu Affiliated Hospital of Qingdao University, Qingdao University
Qingjie Ma China-Japan Union Hospital, Jilin University
Lijuan Niu* Cancer Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College
Wenhai Sun Affiliated Hospital of Qingdao University, Qingdao University
Feng Wang Nanjing First Hospital
Renfei Wang* Tianjin Medical University General Hospital, Tianjin Medical University
Feng Wei First Affiliated Hospital, Baotou Medical College, Inner Mongolia University of Science and Technology
Yu Xia Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Aiming Yang The First Affiliated Hospital of Xi’an Jiaotong University, Xi’an Jiaotong University
Bin Zhang* Peking University Cancer Hospital & Institute
Bo Zhang* Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Guang Zhang* China-Japan Union Hospital, Jilin University
Hong Zhang Sun Yat-sen Memorial Hospital, Sun Yat-Sen University
Li Zhang Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Xiangqian Zheng* Tianjin Medical University Cancer Institute & Hospital, Tianjin Medical University
Review expert committee (listed alphabetically by last name)
Rui An Union Hospital, Tongji Medical College, Huazhong University of Science and Technology
Jugao Fang Beijing Tongren Hospital, Capital Medical University
Youben Fan Shanghai Sixth People’s Hospital, Shanghai Jiao Tong University
Ming Gao Tianjin Medical University Cancer Institute & Hospital, Tianjin Medical University
Zhuming Guo Sun Yat-sen University Cancer Center, Sun Yat-sen University
Gang Huang Shanghai University of Medicine & Health Sciences
Qinghai Ji Fudan University Shanghai Cancer Certer, Fudan University
Ningyi Jiang Sun Yat-Sen Memorial Hospital, Sun Yat-Sen University
Yuxin Jiang Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Anren Kuang West China Hospital, Sichuan University
Fang Li Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Sijin Li First Hospital of Shanxi Medical University, Shanxi Medical University
Yaming Li The First Hospital of China Medical University
Shaoyan Liu Cancer Hospital Chinese Academy of Medical Sciences, Chinese Academy of Medical Sciences
Hui Sun China-Japan Union Hospital, Jilin University
Zhongyan Shan The First Hospital of China Medical University
Jian Tan Tianjin Medical University General Hospital, Tianjin Medical University
Wen Tian Chinese People’s Liberation Army General Hospital
Jing Wang Xijing Hospital, Fourth Military Medical University
Tie Wang Beijing Chaoyang Hospital, Capital Medical University
Xiaoping Xing Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Zhengang Xu Cancer Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College
Fuquan Zhang Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Jiajun Zhao Shandong Provincial Hospital
Yupei Zhao Peking Union Medical College Hospital, Peking Union Medical College, Chinese Academy of Medical Sciences
Jingqiang Zhu West China Hospital, Sichuan University
Secretary(listed alphabetically by last name)
Hui Li Peking Union Medical College Hospital, Peking Union Medical College, Academy of Medical Science
Jiao Li Affiliated Hospital of Qingdao University, Qingdao University
Li Li Peking University International Hospital
Yingjie Zhang Shandong Cancer Hospital & Institute
Teng Zhao Beijing Chaoyang Hospital, Capital Medical University
1.
Sonographic features of persistent/recurrent and metastatic differentiated thyroid cancers (prmDTCs). (A, B) Local recurrence of thyroid bed (among cursors and arrows); (C−E) Suspicious metastatic lymph nodes; (F, G) Recurrence in soft tissue (among cursors); (H) Venous tumor thrombus; (I) Tracheal invasion (arrow point). M, mass; IJV, internal jugular vein; CCA, common carotid artery.