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      Hemosiderin laden macrophages and hemosiderin within follicular cells distinguish benign follicular lesions from follicular neoplasms

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          Abstract

          Background:

          Published criteria to distinguish benign colloid nodules from follicular neoplasms emphasize only three interdependent features: size of follicles, amount of colloid, and cellularity. There is a need for the validation of other independent criteria.

          Methods:

          This study quantified the significance of cystic change, defined as presence of macrophages, and the presence of hemosiderin in either the macrophages or follicular cells. The cohort consisted of 165 patients with fine needle aspiration (FNA) and histologic follow-up of either goiter (101), follicular adenoma (47), or follicular carcinoma (17). Papillary thyroid carcinomas and Hürthle cell neoplasms were excluded from the cohort, because these categories are known to show cystic change and hemosiderin. FNAs were reviewed blindly with the most cellular slide scored for the presence of macrophages and/or hemosiderin.

          Results:

          Hemosiderin within macrophages were seen in 67% (68 of 101) of the goiters and only 6% (four of 64) of follicular neoplasms ( P<.0001). All four follicular neoplasms with hemosiderin in macrophages were adenomas. Three of these four had equivocal features of a benign colloid nodule histologically. None of the 17 follicular carcinomas had hemosiderin in macrophages ( P<.12). Macrophages without hemosiderin also strongly distinguished goiters from neoplasms (83% vs 17%) but appears less useful as a criterion since macrophages were present within 3 of 17 follicular carcinomas. Hemosiderin within follicular epithelial cells was present in 18% (18 of 101) of goiters, whereas none of the 64 follicular neoplasms had intraepithelial hemosiderin ( P<.0003).

          Conclusions:

          If papillary thyroid carcinoma and Hürthle cell neoplasm are ruled out, our findings indicate that the presence of hemosiderin virtually excludes a clinically significant follicular neoplasm.

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          The National Cancer Institute Thyroid fine needle aspiration state of the science conference: a summation

          Introduction On October 22 and 23, 2007, the National Cancer Institute (NCI) hosted "The NCI Thyroid Fine Needle Aspiration (FNA) State of the Science Conference," a two-day gathering in Bethesda, Maryland. Its mission was to establish a comprehensive interdisciplinary informational dialogue dedicated to thyroid FNA. Preparations for the conference began 18 months earlier with the designation of a steering committee, the appointment of nine working committees, coordination with co-sponsoring organizations, and the establishment of a dedicated permanent web site. The function of the website was to serve as a permanent educational tool for health care practitioners and patients alike, as well as to foster on-line dialogue. Six committees were charged with preparing summary documents based on literature reviews on the following subjects: 1. Indications/Pre-FNA requirements; 2. Training and Credentialing; 3. Technique; 4. Terminology and Morphologic Criteria; 5. Ancillary Studies; and 6. Post-FNA Options for Testing and Treatment. Three additional committees were formed, one each to oversee the website, publications ensuing from the conference and the establishment of an on-line educational cytopathology atlas. Literature reviews were limited to English language publications dating back to 1995, using PubMed as the search engine, with key words determined by the committee members. The first draft of the committees' summary documents ("Review and Conclusions") was posted on the web site and open for on-line forum discussion from May 1-June 30, 2007. There were several subsequent drafts and on-line discussion periods (Aug 15 – Sept. 30, 2007 and Nov. 30-Dec. 15, 2007). The documents underwent revision after each comment period prior to re-posting on the web. The two-day "live" conference in October, attended by 154 registrants, comprised of pathologists, endocrinologists, surgeons, and radiologists, gave the committees an in-depth opportunity to present their conclusions and debate controversial areas. This is an abridged version of the topics reviewed at the conference and the website. This is not a "standards of practice" guideline, nor is it endorsed as such by the National Cancer Institute. I. Indications for Thyroid FNA and Pre-FNA Requirements A. Indications for performing an FNA of a thyroid nodule discovered by palpation Every patient with a palpable thyroid nodule is a candidate for fine needle aspiration (FNA) and should undergo further evaluation to determine if an FNA is warranted[1]Thyroid nodules detected by palpation are usually at least 1.0 cm in dimension and are therefore clinically significant. Before a decision is made to perform an FNA, a complete history should be taken; a physical examination directed to the thyroid gland and cervical lymph nodes should be performed; and a serum thyrotropin level (TSH) and thyroid ultrasound (US) should be obtained [1,2]. Patients with a normal or elevated serum TSH level should proceed to a thyroid US to determine if an FNA needs to be performed (see section B below); those with a depressed serum TSH should have a radionuclide thyroid scan, the results of which should be correlated with the sonographic findings [1,2]. Functioning thyroid nodules in the absence of significant clinical findings do not require an FNA because the incidence of malignancy is exceedingly low [3]. A nodule that appears either iso- or hypo-functioning on radionuclide scan, however, should be considered for FNA based on US findings (see section B below) [1]. B. Indications for performing an FNA of a thyroid nodule discovered via imaging A nodule not previously suspected or discovered clinically, but detected by an imaging study, is considered an incidental nodule ("incidentaloma"). Incidentalomas detected by 18FDG-PET are unusual (2–3% of all PET scans) but have a higher risk of cancer (14–50%) compared to background incidence [4]. Therefore, a focal nodule that is 18FDG-PET-avid is an indication for FNA. This applies only to focal lesions. Diffuse increased uptake on 18FDG-PET does not warrant FNA unless thyroid sonography detects a discrete nodule. All focal hot nodules detected on sestamibi scans and confirmed by US to be a discrete nodule should undergo FNA. Thyroid incidentalomas detected on sestamibi scans have a higher risk of cancer (22–66%) compared to baseline risk [5,6]. Incidentalomas detected by US (e.g., carotid Doppler scans or scans done for parathyroid disease) have a cancer risk of approximately 10–15% (0–29%) and should undergo dedicated thyroid sonographic evaluation [7-12]. Lesions with a maximum diameter greater than 1.0–1.5 cm should be considered for biopsy unless they are simple cysts or septated cysts with no solid elements. FNA may also occasionally be replaced by periodic follow-up for nodules of borderline size (between 1.0 and 1.5 cm in maximum diameter) if they have sonographic features that are strongly associated with benign cytology. A nodule of any size with sonographically suspicious features can also be considered for FNA. Sonographically suspicious features include microcalcifications, hypoechoic solid nodules, irregular/lobulated margins, intra-nodular vascularity, and nodal metastases (or signs of extracapsular spread). This latter recommendation is controversial because it includes patients with microcarcinomas, in whom a survival benefit following an FNA diagnosis has not been documented. Nevertheless, the American Thyroid Association, the Academy of Clinical Thyroidologists and a collaborative effort of the American Association of Clinical Endocrinologists and the Associazione Medici Endocrinologi make this recommendation [1,7,13]. There are few direct data on the cancer risk of thyroid incidentalomas detected by computed tomography (CT) or magnetic resonance imaging (MRI). They are seen in at least 16% of patients evaluated by neck CT or MRI [14]. The risk of cancer in one study was predicted at 10%, but it included only a limited number of patients who went on to FNA[15]. CT and MRI features can not determine the risk of malignancy, except in very advanced cases that are unlikely to be incidental. Until more data are available, incidentalomas seen on CT or MRI should undergo dedicated thyroid sonographic evaluation. Any nodule with sonographically suspicious features (see above) should be considered for FNA. In addition, lesions that have a maximum diameter greater than 1.0–1.5 cm should also be considered for FNA (see above). C. Indications for performing a thyroid FNA using palpation vs. ultrasound for guidance In the evaluation of individual patients with nodular disease, there are occasions when either palpation or ultrasound-guided (US-guided) FNA of a thyroid nodule are reasonable to perform. Palpation-guided FNA can be performed with high levels of success in specific circumstances [16-18]. The benefits of palpation-guided FNA of thyroid nodules are its reduced cost in comparison to US-guided FNA as well as its logistical efficiency: the practitioner can perform the procedure without an US machine or assistance from other practitioners. Published data from one study concludes that US evaluation changes the management of 63% of patients with palpable thyroid nodules [19]. US findings like irregular margins, microcalcifications, intra-nodular vascularity and the characteristics of other occult thyroid nodules can be used to identify nodules at risk that should be sampled [12,20]. In several studies US guidance was shown to reduce the rates of non-diagnostic (i.e., insufficient cells and/or colloid) and false-negative aspirates [16,17,21]. Re-evaluation of patients using US-guided FNA for those with initially benign results on palpation-guided FNA, led to the reclassification of patients and the diagnosis of 14% more cancers in one series [22]. Finally, there are US-specific findings that can be used to inform the results of the US-guided FNA (e.g. the benign sonographic appearance of a unilocular cyst explains why only cyst fluid was obtained by FNA). A palpation-guided FNA can be considered when a thyroid nodule >1 cm in maximum diameter has been confirmed via US examination of the thyroid. The sonographic examination is important, because physical examination can be imprecise in determining nodule size, its origin from the thyroid rather than adjacent tissues, and the degree of cystic change. US-guided FNA is acceptable and is preferred for nodules that are not palpable, >25% cystic or have been biopsied before and yielded a non-diagnostic result [23,24]. D. The informed consent form for thyroid FNA Legislation regulating the conditions under which consent must be obtained vary greatly by state [25-27]. Thus, providers (e.g., pathologists, radiologists, surgeons, endocrinologists, etc.) who perform thyroid FNA need to design informed consent policies and forms based on state regulations. For thyroid FNA, informed consent materials, including written documents, if used, should describe the FNA procedure and potential risks and complications. The possibility of the most frequently occurring complication, namely, hematoma, should be mentioned. Information should be presented in a manner to facilitate patient understanding. It might be useful to mention the possibility of a non-contributory result. Estimates of accuracy, such as false-negative and false-positive proportions, are not mandatory and should be considered only if the practitioner believes they would facilitate patient comprehension. E. Information required on the requisition form that accompanies a thyroid FNA Federal regulations in the United States require that specific identifying information be provided to laboratories with all specimens submitted for laboratory testing [28]. These include the name and address of the person requesting the test; the patient's name or unique identifier; the patient's gender; the patient's age or date of birth; the name of test to be performed; the specimen source; the date of specimen collection; and any additional relevant information. The purpose of this discussion is to consider what 'additional relevant information' a laboratory needs to properly evaluate a thyroid FNA specimen. The location of the nodule (right vs. left; isthmus; upper pole, mid-pole, lower pole, etc.) should be specified on the requisition form to permit correlation with sonographic findings and subsequent histopathologic examination (if any). Such identification is often necessary because patients often present with multiple nodules (some but not all of which may be biopsied), or they may develop other nodules over time. There is, at best, an imperfect correlation between the size of a nodule and the likelihood of malignancy, but larger nodules (>4 cm) may be associated with a higher malignancy risk, and therefore size should be included [29]. Benign cytologic changes that mimic malignancy, particularly papillary carcinoma, occur in some patients with autoimmune (Hashimoto's) thyroiditis. If not alerted to this history, a misdiagnosis can occur. Furthermore, nuclear alterations may be seen in patients with a history of I-131 therapy (for hyperthyroidism) or external radiation [30]. In some patients with Graves' disease, an FNA of a nodule may include pleomorphic cells from the extra-nodular Graves' thyroid parenchyma that can be a pitfall in cytologic interpretation [31]. It is important to note a personal history of malignancy because metastatic tumors to the thyroid can mimic the appearance of a primary thyroid neoplasm. Metastatic renal cell carcinoma mimics a follicular neoplasm; melanoma can mimic medullary carcinoma; metastatic lung cancer can mimic anaplastic carcinoma of the thyroid. Cytologists should be alerted to the possibility of a metastatic tumor in any patient with a history of malignancy. Approximately 15% of medullary thyroid cancers are familial (familial MTC or MEN2a or 2b). Knowledge of family history can alert the pathologist to the possibility of medullary carcinoma. Recent data show that papillary thyroid cancer can also be familial, and thus knowledge of such family history can alert the pathologist to consider papillary carcinoma. Therefore, at a minimum, the following data should appear on the requisition form that accompanies a thyroid FNA to the laboratory: 1. Usual required data for lab test submission (see above) 2. Location of the nodule 3. Estimated size of the nodule 4. History of hypothyroidism, autoimmune thyroiditis, or a positive test for anti-thyroid antibodies 5. History of Graves' disease 6. History of I131 or external radiation therapy, accompanied by the dates of treatment 7. Personal history of cancer 8. Family history of thyroid cancer The following information can be useful to the cytologist but is considered optional on the requisition form: 1. additional clinical history, e.g., that a prior FNA was done, or that the patient is undergoing levothyroxine therapy. Morphologic alterations due to a prior FNA can affect cytologic interpretation, and levothyroxine use can alter follicular cell morphology. 2. TSH level. If a patient has Hashimoto's hypothyroidism or Graves' disease, cytologic findings can be affected. A lower serum TSH level is also associated with a lower risk of thyroid cancer. 3. results of US examination. 4. results of nuclear medicine imaging studies[32,33]. II. Training and Credentialing for the Performance of a Thyroid FNA A. Training for the Performance of Thyroid FNA Diagnostic accuracy of thyroid FNA is highly variable [18,34-38]. The majority of diagnostic failures are due to non-diagnostic samples or pathologists issuing diagnosis on samples with inadequate material [39]. Efforts toward improvement in proficiency in FNA sampling and specimen preparation should be given high priority. Reports comparing the effectiveness of specific, defined training strategies for FNA procurement are lacking and there is little agreement on what the definition of adequate training is. Merely performing a large number of FNAs does not improve results when controlled for level of training[40]. There is, however, evidence that when FNA specimen procurement is concentrated in fewer hands and when the same physician both procures and microscopically examines the specimen, the results improve [41,42]. Training in procurement has significant impact on results regardless of the method of guiding the needle (ie palpation vs. ultrasound guidance). The consistent and timely feedback on specimen quality provided to physicians who both procure and examine specimens microscopically helps to improve results as well. Ultrasound (US) guidance of the sampling provides evidence that the needle is correctly placed within the target. Two reviews of FNA state that the procurement of the samples is not as easy as generally perceived and stress the importance of obtaining an adequate sample in order for the test to be useful [41,43]. Suen makes the recommendation that "the procedure is carried out by a core group of dedicated physicians" [44]. In a 2003 editorial Kocjan discussed many of the problems associated with the current practice of FNA and stressed the importance of training in specimen collection and preparation regardless of the specialty of the operator[45]. A recent publication on the teaching of procedural skills indicates that the most important factor for mastering procedures is focused training with appropriate feedback by expert practitioners [46]. The previously widely held belief that simply performing a large number of procedures produces excellence does not appear to be true [47]. Given these observations it doesn't make sense to advocate that a specific number of procedures should be performed without specifying the circumstances. Reports comparing the effectiveness of specific, defined training strategies for FNA sampling are lacking in the literature. Such studies would be helpful in order to optimize training of operators in various settings and specialties. In addition to the harvesting of diagnostic material, training for technical excellence in sample preparation cannot be overemphasized. Several options are available for the preparation and processing of FNA specimens. On-site sample adequacy assessments are performed with smears which may be stained with a modified Giemsa or a rapid Papanicolaou technique. In order to optimize on-site adequacy smears, appropriate training in smear technique is imperative in any FNA training program regardless of specialty. On-site evaluation of the specimen adequacy has lessened the percent unsatisfactory specimens and limited the number of passes per nodule sampled [48-50]. In all but one of these reports on-site evaluation of the specimens was one of several factors reported to improve accuracy, but was not calculated as a separate factor [50]. One report found on-site evaluation helpful in minimizing unsatisfactory samples only for less experienced radiologists procuring samples [51]. At the very least, it appears that on-site evaluation serves as an important educational tool for the physician performing the FNA in providing immediate feedback on the quality of the specimen. Training in US imaging technique and interpretation is beyond the scope of this review. Components of FNA procurement training: 1. Studying of texts and DVD or similar teaching aids with moving images that explain the principles and show all required tasks including sampling and specimen preparation in detail. Lectures and demonstrations can also be helpful. A detailed instructional video done by Dr. Britt-Marie Ljung is available to all, sponsored by the Papanicolaou Society of Cytopathology on their website under the PSC Guidelines link. 2. Bench practice of sampling and smearing on bovine liver or similar safe material, under supervision. Timely and precise placement of the needle tip under ultrasound guidance can be practiced with a model (for example turkey breast with a "target" inserted between the muscles or commercially available practice materials). 3. Sampling of thyroid nodules guided either by palpation or US, supervised by a proficient operator, and followed by examination of all samples to provide timely feed back on quality of samples. 4. Number of cases needed for achieving proficiency will vary depending on individual background and aptitude as well as case mix. Although it is best to start with easier cases, challenging cases need to be included. One should expect at least 90% diagnostic specimens before training is complete. The sampling of thyroid cysts devoid of follicular cells designated as "cyst fluid only" and categorized as " non-diagnostic" should not be considered "non-diagnostic" for credentialing purposes. B. Credentialing and re-credentialing Complete residency/fellowship training including FNA procurement or equivalent training in an alternative setting should suffice for initial credentialing. For re-credentialing, documentation of the number of total FNA procedures per year, for an individual provider, in combination with a documented unsatisfactory sample rate ( 50% of nodules which are non-diagnostic or indeterminate on initial cytologic diagnosis can latter be placed into definite diagnostic categories with repeat FNA [71,73]. Follicular neoplasm/Suspicious for follicular neoplasm This term encompasses both benign and malignant tumors; i.e. follicular adenoma and carcinoma. The FNA of a follicular neoplasm usually shows: • Hypercellularity as compared to most aspirates of nodular goiter demonstrating a monotonous population of follicular cells with minimal or absent background colloid. The cells are usually arranged in three dimensional groups and microfollicles with prominent nuclear overlapping and crowding. Some cases may show nuclear atypia; however, this is not a diagnostic criterion of malignancy, since benign nodules can also show nuclear atypia [84]. • The presence of microfollicles in an FNA specimens may be diagnostic of a follicular lesions neoplasm (adenoma or carcinoma) [85]. Some authors have proposed the term micro-follicular lesion [75]. However, various studies have shown that the interpretation of microfollicles suffers from inter-observer variability. Additionally, aspirates of normal thyroid and hyperplastic/adenomatoid nodules can show microfollicles [86]. Others have suggested that diagnosis of follicular neoplasm should only be used when a thyroid FNA specimen demonstrates a monotonous cell population arranged in cohesive groups with nuclear overlapping and crowding in a background if thick instead of watery colloid [80]. Hurthle cell neoplasm FNA specimens of Hürthle cell lesions (benign and malignant) usually show: • Cellular aspirate comprising a single cell population of Hürthle cell in a background of minimal colloid. Cells can be arranged in monolayer sheets, follicular groups or as scattered single cells [87]. Some authors have suggested that cellular dispersion leading to single cells is more common in aspirates of Hurthle cell carcinoma than adenoma; however, this observation has not been validated [87]. Cellular atypia is also commonly observed in Hurthle cell lesion; this can be seen in the form of random nuclear enlargement, multi-nucleation, cellular pleomorphism and prominent nucleoli. • FNA specimens of neoplastic Hurthle cell lesions may show intra-cytoplasmic lumens and transgressing vessels [88]. Follicular Variant of Papillary Carcinoma Similar to the histologic diagnosis the cytologic interpretation of FVPTC can also be difficult. The FNA specimens of FVPTC usually show: • Tumor cells arranged in monolayer sheets and follicular groups in a background of thin colloid. Thick colloid can also be present, however, much less as compared to classic PTC. The tumor cells show nuclear elongation, chromatin clearing and thick nuclear membranes; however, nuclear grooves and inclusions are rare. Nonetheless, chromatin clearing and nuclear membrane thickening is always seen in these cases [89,90]. • If a thyroid FNA specimen focally shows cells with nuclear elongation, chromatin clearing and grooves but lacks nuclear inclusions, it may be diagnosed such as "follicular neoplasm with features suspicious for PTC. 3. Morphologic Criteria of Malignant Tumors The well-differentiated thyroid carcinomas are the commonest form of malignant thyroid tumors. They are more common in young adults, whereas, the less differentiated and anaplastic tumors of the thyroid are prevalent in older age. Cytology of Papillary Thyroid Carcinoma (PTC) and its variants The cytologic features of PTC can be divided into major and minor diagnostic features; these are as follows: • Major Diagnostic Criteria: Enlarged, oval "and irregular" nucleus, eccentric and often multiple micro-nucleoli, fine, pale chromatin, longitudinal intranuclear grooves and intranuclear pseudo-inclusions [76,91]. • Minor Diagnostic Criteria: Papillary cyto-architecture, syncytial monolayers, dense squamoid cytoplasm, "Bubble gum" colloid, psammoma bodies, multinucleated giant cells, histiocytoid cells and cellular swirls [92-94]. Follicular variant of papillary carcinoma: Refer to section on follicular patterned lesions of thyroid. Tall cell variant of papillary carcinoma Cytology specimens of this tumor usually show elongated cells with sharp cytoplasmic borders, granular eosinophilic cytoplasm and variably sized nuclei with nuclear features of papillary carcinoma. The nuclear features of papillary carcinoma are usually abundant and readily identifiable as compared to other variant of PTC [95]. Medullary Thyroid Carcinoma The FNA specimens from MTC can show varied morphologic pattern similar to that seen in surgical pathology specimens. The majority of MTC cases show: • A cellular aspirate consisting of round to oval cells arranged mainly as single cells or loosely cohesive groups. The individual tumor cells show abundant eosinophilic granular cytoplasm and up to 20% of cells will demonstrate fine granules in Romanowsky-stained preparations. The nuclei are usually eccentric giving rise to a plasmacytoid appearance to tumor cells. • The nuclear chromatin is similar to that seen in neuroendocrine tumors; salt and pepper type with inconspicuous nucleoli. Intranuclear inclusions and multinucleated cells can also be seen. • In some cases of MTC the tumor cells are can assume a "spindle shape" and appear mesenchymal in origin. Amyloid may be observed as acellular material in the form of strings or as round to oval shaped fragments. • In cytology specimens the diagnosis of MTC can be confirmed by performing immunostains for Calcitonin. In cases with limited cellularity it is advisable to have a serum Calcitonin levels performed on the patient to confirm the diagnosis of MTC [76,96]. Anaplastic carcinoma The aspirates from anaplastic carcinoma usually do not pose any diagnostic difficulties; they can be readily classified as malignant due to extreme cellular pleomorphism and obvious malignant features [97,98]. V. Utilization of Ancillary Studies in Thyroid FNA A. Indications for ancillary studies in thyroid FNA Medullary carcinoma and anaplastic carcinoma are the most common primary thyroid tumors that may require additional immunohistochemical studies to confirm the diagnosis. Although rare, metastatic tumors may occur in the thyroid and a history of a known primary along with a pertinent immunohistochemical panel would be helpful in making a final diagnosis. The utilization of ancillary studies to re-classify an indeterminate or suspicious FNA into a benign or malignant category or to refine the risk of malignancy within this category is controversial. B. Specific ancillary studies to be performed for each of these indications The ancillary studies with the widest utility involve the detection of specific proteins using immunologic techniques, typically immunohistochemistry on cell block preparations. Immunocytochemistry may also be utilized but only after careful validation of the protocols for this type of specimen. In cases of suspected medullary carcinoma, an immunohistochemical panel of calcitonin, thyroglobulin, CEA, and chromogranin can be confirmatory. Immunohistochemical findings should be correlated with serum calcitonin levels, particularly if there is insufficient FNA sample for ancillary studies [99-106]. Care should be employed in evaluating the results of calcitonin staining on cell block preparations of thyroid neoplasms with oncocytic features as cases of non-specific staining of oncocytic cells have been documented. Endogenous biotin in follicular cells may also cause non-specific staining. Anaplastic carcinoma is often apparent based on its pleomorphic cytomorphology and aggressive clinical presentation. Anaplastic carcinoma often lacks TTF-1 and thyroglobulin staining. However, IHC for pan-cytokeratin may be utilized to distinguish anaplastic carcinoma from sarcomas. The clinical setting may also raise the possibility of a metastatic lesion [107-112]. The most common metastases to the thyroid arise from primary carcinomas of the kidney, lung, breast, colon, or malignant melanoma. The clinical history and presentation is important in determining the appropriate ancillary studies. One may initially employ TTF-1 and thyroglobulin IHC to narrow the primary site to thyroid, followed by further IHC characterization if these stains are negative [113]. One challenging area is excluding the possibility of lymphoma in the setting of Hashimoto's thyroiditis. All cases of Hashimoto's thyroiditis should not be automatically sent for flow cytometric immunophenotyping. In addition, immunophenotyping results from thyroid FNA samples should be interpreted with caution since Hashimoto's thyroiditis may yield κ/λ ratios that are skewed beyond normal values associated with reactive lymph nodes [114]. The indication for flow cytometric immunophenotyping should be based on cytomorphologic or clinical features that raise the suspicion of lymphoma. Parathyroid tissue can be extremely difficult to distinguish from thyroid tissue based on cytomorphologic features alone. In this setting, IHC for TTF-1, PTH, and chromogranin may be helpful. Neither the IHC nor the cytomorphology should be utilized to distinguish normal from abnormal parathyroid tissue. Chemical detection of PTH levels in FNA samples has been utilized, and may be considered following careful assay validation [115-120]. The identification of metastatic thyroid carcinoma to a lymph node in patients with a known history of thyroid carcinoma is often straightforward based on cytologic features. In challenging cases, IHC for TTF-1, calcitonin, and thyroglobulin may be useful in identifying the thyroid as a primary site for the nodal metastasis. Several studies have addressed the utilization of chemical assays for thyroglobulin on the FNA sample from neck lymph nodes [121,122]. Such an approach should be implemented with caution since clinical management of patients with benign or indeterminate lymph node FNAs containing detectable thyroglobulin remains undefined. Ancillary studies that would permit re-classification of an indeterminate or suspicious thyroid FNAs into a benign or malignant category are highly desirable. Potential thyroid carcinoma-associated molecular markers include proteins (galectin-3, Cytokeratin-19, HBME-1), chromosomal translocations (RET/PTC, PAX8/PPARG), and genetic mutations (BRAF, RAS) [123-125]. This review has focused on molecular markers that have proven efficacy for the above stated indication. The specificity of several markers for thyroid carcinoma is promising, but based on current limited evidence, widespread clinical use will require further studies. The indications for performing ancillary studies and the current state of the science for ancillary studies in thyroid FNA are summarized in Table 2. Table 2 Review of Utilization of Ancillary Studies in Thyroid FNA Suspected medullary carcinoma  • IHC panel (calcitonin, thyroglobulin, CEA, chromogranin)  • Serum calcitonin Suspected anaplastic carcinoma  • IHC for pan-cytokeratin Suspected metastatic carcinoma  • IHC for TTF-1 (If TTF-1 negative, then expand IHC panel based on cytomorphology and clinical setting to identify primary) Suspected lymphoma  • Flow cytometric immunophenotyping Suspected parathyroid lesion  • IHC for TTF-1, PTH, chromogranin  • May consider PTH level assessment on FNA sample Suspected metastatic thyroid carcinoma to lymph node  • IHC for TTF-1, thyroglobulin, calcitonin  • May consider thyroglobulin level assessment on FNA sample Atypical/Borderline/Suspicious FNA  • No specific tests based on insufficient evidence C. Sample preparation for each type of ancillary study If IHC is anticipated, one dedicated pass should be performed for cell block preparation from an FNA sample. The routine use of thyroid core biopsy to perform IHC is not supported. If lymphoma is suspected, at least one dedicated pass in a supportive medium should be obtained for flow cytometric analysis. Ancillary studies to detect genetic alterations may require dedicated passes and special processing protocols depending on the analyte (DNA or RNA) and the methodology (FISH, PCR, RT-PCR). VI. Post FNA Options for Testing and Treatment A. Follow-up of "Non-diagnostic" FNA Results A universally accepted approach to "Non-diagnostic" thyroid FNAs is currently lacking. The strategy reviewed here is based on the American Thyroid Association's proposal, recent literature and the NCI Conference on Thyroid FNA [9,48]. Non-diagnostic aspirates obtained from cystic and solid nodules are treated differently in follow-up strategies. Aspirates composed of pure colloid and lacking a cellular component are considered benign, but require close clinical and ultrasound follow-up. Aspirates of cysts containing blood and histiocytes but no epithelial component need correlation with ultrasound findings [19]. Many cystic nodules contain only colloid surrounded by a thin rim of benign epithelium. These cysts are at very low risk for harboring malignancy. Many authors recommend these cysts be managed by nonsurgical follow-up. Other authors point to the low, but real incidence of papillary carcinoma in cysts and recommend surgical resection after two "Non-diagnostic" aspirations. The timing of repeat needle aspiration has not been established, but 6 to 18 months appears reasonable. Cystic lesions with a "Non-diagnostic" aspirate should undergo repeat FNA if ultrasound demonstrates suspicious areas [12,126]. The repeat FNA should be under ultrasound guidance and, when possible, intraprocedural review of the aspirated material by a cytopathologist is recommended [48,19]. When repeat FNA yields "Non-diagnostic" material, correlation with family history, close clinical and ultrasonographic follow-up is suggested [19]. Solid nodules with a "Non-diagnostic" aspirate should be re-aspirated with ultrasound guidance with, if possible, intraprocedural review by a cytopathologist. If repeat smears are "Non-diagnostic," surgery ought to be considered. If the patient is likely to return for follow-up and the nodule is 1 cm or less in size, close clinical follow-up with ultrasound examination is a reasonable alternative to surgery [19]. When growth of the nodule is detected during surveillance, excision is suggested but repeat FNA is an acceptable approach. In general, for both solid and cystic "Non-diagnostic" aspirates a waiting period of at least three months should elapse between the initial "Non-diagnostic" aspirate and reaspiration. If suspicion for carcinoma is high based on clinical or ultrasonographic findings, a shorter waiting period may be appropriate. B. Follow-up of "Benign" FNA Results Management of patients with a "Benign" FNA diagnosis has varied between institutions. Because cytologically benign thyroid nodules are associated with up to 5% false negatives, these nodules require careful follow-up [16,127]. Patients with multiple thyroid nodules have the same risk of malignancy as those with a single nodule. Follow-up of patients with multiple nodules should be the same as those with a solitary nodule. Certain ultrasonographic characteristics (microcalcification, hypoechogenicity, intranodular hypervascularity) indicate a higher likelihood of malignancy [12,126]. Nodules with these features require more frequent clinical and ultrasonographic follow-up after a benign FNA. The false negative rate may be higher when FNAs are directed by palpation rather than by ultrasound [17,128,129]. Thus, palpation directed FNAs may require closer follow-up. Medical suppressive therapy to confirm a benign cytologic diagnosis remains controversial. Multiple randomized trials have shown that thyroid hormone suppression may result in a decrease in nodule size in patient populations with borderline low iodine intake. The data are less convincing for populations ingesting sufficient iodine [130-132]. Rare examples of carcinomas suppressed by thyroid hormone have been reported. It is unclear that thyroid suppressive therapy is a reliable test for confirmation of a benign cytologic diagnosis of a solitary nodule. Cytologically benign nodules can be followed clinically with interval ultrasound examination [19]. Benign nodules may be reaspirated or surgically removed when significant changes occur in their ultrasonographic appearance. Ultrasonography appears to be the best technique for detection of changes in nodule size[133]. There is no general agreement as to what constitutes a significant increase in nodule size. The American Thyroid Association (ATA) has suggested that a 20% increase in nodule diameter with a minimum increase in two or more dimensions of at least 2 mm is a reasonable definition for a significant change in nodule size [9]. The ATA has also recommended clinical follow-up of cytologically benign and easily palpable nodules occur at 6–18 month intervals. When nodules are not easily palpable, the recommendation is for serial ultrasound examinations at 6–18 month intervals [9]. Thyroid nodules cytologically diagnosed as benign require careful clinical follow-up. Easily palpable nodules may be followed clinically at 6–18 month intervals. Nodules which are not easily palpable should receive serial ultrasound examinations at 6–18 month intervals. The total duration of the follow-up period should be at least 3–5 years. When a 20% increase in nodule diameter or a minimum of 2 mm increase in two dimensions is detected, repeat FNA is performed. Repeat FNA should be performed if ultrasound abnormalities (irregular margins, central hypervascularization) develop. The repeat FNA should be under ultrasound guidance. Attendance of a pathologist at reaspiration is desirable. At this time, hormone suppressive therapy can not be recommended as a diagnostic maneuver for confirmation of benignity in a cytologically benign thyroid nodule. Ethanol ablation may be considered in selected patients. C. Follow-up of FNA specimens diagnosed as "Follicular lesion/Atypical/Borderline" A variety of terms are employed to convey uncertainty about the significance of some thyroid cytologic findings. Such changes do not rise to the level of a significant concern for a follicular neoplasm meriting lobectomy (see section D), nor do they fit a "Suspicious for Malignancy" interpretation. Because of cytologic or architectural atypia, neither can such cases be reliably called benign. A variety of diagnostic headings are used for such cases including "Atypical Follicular Lesion", "Cellular Follicular Lesion" and "Indeterminate" [73,134]. The term "Atypical/Borderline" will be used for this discussion. Approximately 5–10% of the "Atypical/Borderline" category are malignant neoplasms. Given that this diagnostic category is associated with low specificity and a low positive predictive value, the appropriate follow-up for this category remains controversial. Some authorities have recommended repeat FNAs, repeat ultrasound scans, or repeat radio-nucleotide uptake studies. A repeat FNA is benign in about one-half of patients, obviating the need for surgery [71]. Radiological correlation may aid in improving the overall positive predictive value of this category. Besides increasing size, ultrasonographic features such as hypoechogenicity, irregular border, calcifications and abnormalities of vascularization all favor a malignant diagnosis [54,135]. Outside expert cytopathology consultation may be considered in cases with an "Atypical/Borderline" cytologic diagnosis. In general, a conservative approach may be taken. After a single "Atypical/Borderline' interpretation, a repeat FNA should be considered in 3 to 6 months. If the repeat FNA is "Atypical/Borderline" or worse, a surgical consultation should be considered [71]. D. Follow-up of an FNA with the diagnosis of "Neoplasm (Follicular)" This category has, in some reports, been termed "Suspicious for Follicular Neoplasm" [54,71]. The majority of cases in this category are adenomas, but 20 to 30% are carcinomas [73]. Patients with a diagnosis of "Follicular Neoplasm" should be referred for operative exploration. Usually a lobectomy is performed followed by histologic examination for capsular and vascular invasion. The utility of frozen section evaluation for capsular or vascular invasion is controversial. Most participants at the NCI Meeting voiced the opinion that frozen section evaluation does not play a role in the separation of follicular adenoma from follicular carcinoma. Some surgeons may perform frozen section to determine the necessity for additional surgery, but there is no published data to support this practice. When frozen section is not utilized, initial surgery is lobectomy. If subsequent histologic examination discloses capsular or vascular invasion, the diagnosis of follicular carcinoma is made. Depending on the surgeon's discretion, histopathologic findings and clinical status of the patient reoperation with thyroidectomy may be performed. E. Follow-up of FNAs with a diagnosis of "Suspicious for Malignancy" Approximately 50–75% of lesions cytologically diagnosed as "Suspicious for Malignancy" are papillary carcinomas [71,73,134]. Less commonly, other malignancies such as medullary carcinoma are included in this category. Patients with an FNA diagnosis of "Suspicious for Malignancy" should be referred for thyroid lobectomy. Subsequent operative intervention depends on histological review. F. Follow-up of "Malignant" FNA Results This category refers to the histopathologic entities of papillary carcinoma, medullary carcinoma, lymphoma and anaplastic carcinoma. A comprehensive review of this subject concluded that the cytologic diagnosis of malignancy in a thyroid nodule should result in surgical consultation. Whenever possible, the type of carcinoma present should be stated in the cytology report. If a metastatic carcinoma is suspected, clinical and imaging studies should be undertaken to establish the primary site. At the surgeon's discretion, surgical intervention may initially be simple lobectomy or intraoperative frozen section examination to determine if total thyroidectomy should be performed. If frozen section is equivocal, the operative procedure is ended with lobectomy and further therapy is based on permanent sections. Depending on the surgeon's discretion and the characteristics of the malignancy, total thyroidectomy may be performed for a cytological diagnosis of papillary carcinoma. Controversy exists as to whether total thyroidectomy or unilateral lobectomy should be performed for papillary carcinoma. The selection of lobectomy versus thyroidectomy depends on the evaluation of the patient's clinical status and the size and nature of the papillary carcinoma. Total thyroidectomy may be accompanied by a central compartment dissection. For patients with large, bulky disease or recurrent laryngeal nerve dysfunction, preoperative cross sectional imaging should be considered as well as ultrasound imaging for lateral neck nodal disease. Competing interests The author(s) declare that they have no competing interests.
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            Common and uncommon sonographic features of papillary thyroid carcinoma.

            To determine the relative frequency of various sonographic findings in papillary carcinoma of the thyroid. We retrospectively analyzed the sonographic features in 55 patients with proven papillary carcinoma of the thyroid. Sonographic features analyzed were echo texture, cystic change, margin, contour, presence of a peripheral halo, vascularity, and calcification pattern. Features were classified as common (> or = 35% of cases) or uncommon (< 10% of cases). Combinations of features were also analyzed. Common sonographic features of papillary carcinoma included hypoechoic texture (86%), microcalcifications (42%) or no calcifications (47%), well-defined margins (47%), and intrinsic hypervascularity (69%). Uncommon features included hyperechoic or mixed echo texture, cystic elements, irregular margins, hypovascularity, and coarse or peripheral calcifications. Of the 29 lesions that had calcifications, 20 (69%) had microcalcifications; 5 (17%) had coarse calcifications; and 1 had peripheral calcifications. In total, 54% of cases had at least 1 uncommon feature, and 11% had 2 or more uncommon features. Cystic carcinomas were rare and accounted for only 6% of lesions; all had hypervascular solid components. No carcinomas in our series were completely avascular. There is a broad spectrum of sonographic findings in papillary carcinoma of the thyroid. Half of the lesions in this series had at least 1 uncommon sonographic feature.
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              Fine-needle aspiration biopsy of thyroid nodules: advantages, limitations, and effect.

              The efficacy of fine-needle aspiration (FNA) biopsy and its role in the management of a nodular goiter are clearly established. The accuracy of cytologic diagnosis approaches 95%. FNA biopsy is a reasonable approach to thyroid nodules; it has decreased costs substantially because it facilitates selection of patients who need to undergo surgical excision. Selecting patients for operation on the basis of results of FNA biopsy has more than doubled the yield of carcinoma. The limitations of cytologic examination, nondiagnostic results, and cellular follicular neoplasms should be remembered but need not negate continued use of FNA biopsy. Negative (benign) and positive (malignant) cytologic results are conclusive; careful clinical follow-up of benign nodules and surgical excision of malignant nodules are recommended. Nondiagnostic results are inconclusive; further evaluation by repeated FNA biopsy, ultrasound-guided biopsy, or radionuclide scanning is necessary. Suspicious cytologic results are also inconclusive and are associated with a 20% chance of malignant involvement; surgical treatment is necessary for clarification. The role of levothyroxine therapy remains uncertain and is not recommended until compelling data are available. FNA biopsy is a safe, simple, reliable, and cost-effective means of detecting benign nodules. FNA biopsy, not thyroid scanning or ultrasonography, is the preferred initial diagnostic test in all patients with thyroid nodules.
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                Author and article information

                Journal
                Cytojournal
                CJ
                Cytojournal
                Medknow Publications (India )
                0974-5963
                1742-6413
                2009
                19 January 2009
                : 6
                : 3
                Affiliations
                Department of Anatomical Pathology, University of Massachusetts, MA USA
                Article
                CJ-06-45193
                10.4103/1742-6413.45193
                2678825
                19495407
                8e0ed0a4-28a9-4f9f-9e3c-82753cd38998
                © 2009 Jaffar et al; licensee Cytopathology Foundation Inc.

                This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

                History
                : 16 September 2008
                : 02 December 2008
                Categories
                Original Article

                Clinical chemistry
                hemosiderin laden macrophages,macrophages,hemosiderin within follicular neoplasms,follicular cells,benign colloid nodule

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