Genome-Wide Appraisal of Thyroid Cancer Progression

Wreesmann, Volkert B.; Ghossein, Ronald; Patel, Snehal G.; Harris, Chad; Schnaser, Erik; Shaha, Ashok R.; Tuttle, R. Michael; Shah, Jatin P.; Rao, Pulivarthi H.; Singh, Bhuvanesh

doi:10.1016/s0002-9440(10)64433-1

Cited by 155 publications

(132 citation statements)

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“…Indeed, our group showed that the median number of chromosomal abnormalities per case rises from 1 in well-differentiated PTC to 10 in anaplastic carcinoma, with intermediate values of 3 and 5 for TCV and PDTC, respectively. 17 In a minority of cases, morphologic instability was best demonstrated in cases in which the metastasis demonstrated a betterdifferentiated histology compared with the primary tumor. This phenomenon has been previously reported in bone metastases from thyroid carcinomas.…”

Section: Discussionmentioning

confidence: 99%

Histopathologic characterization of radioactive iodine‐refractory fluorodeoxyglucose‐positron emission tomography‐positive thyroid carcinoma

Rivera

Ghossein

Schöder

et al. 2008

Cancer

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191

130

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BACKGROUND.Radioactive iodine‐refractory (RAIR) 18F‐fluorodeoxyglucose (FDG)‐positron emission tomography (PET) positive thyroid carcinomas represent the major cause of deaths from thyroid carcinomas (TC) and are therefore the main focus of novel target therapies. However, to the authors' knowledge, the histology of FDG‐PET‐positive RAIR metastatic thyroid carcinoma has not been described to date.METHODS.Metastatic tissue from RAIR PET‐positive patients identified between 1996 and 2003 at the study institution were selected for histologic examination. The biopsied metastatic site corresponded to a FDG‐PET positive lesion sampled within 2 years (87% of which were sampled within 1 year) of the PET scan. Detailed microscopic examination was performed on the metastatic deposit and the available primary tumors. Poorly differentiated thyroid carcinomas (PDTC) were defined on the basis of high mitotic activity (≥5 mitoses/10 high‐power fields) and/or tumor necrosis. Other types of carcinomas were defined by conventional criteria. The histology of the metastases and primary were analyzed, with disease‐specific survival (DSS) as the endpoint.RESULTS.A total of 70 patients satisfied the selection criteria, 43 of whom had primary tumors available for review. Histologic characterization of the metastasis/recurrence in 70 patients revealed that 47.1% (n = 33 patients) had PDTC, 20% (n = 14 patients) had the tall cell variant (TCV) of papillary thyroid carcinoma, 22.9% (n = 16 patients) had well‐differentiated papillary thyroid carcinoma (WDPTC), 8.6% (n = 6 patients) had Hurthle cell carcinoma (HCC), and 1.4% (n = 1 patient) had anaplastic carcinomas. The histopathologic distribution of the tumor in the primaries was: PDTC, 51%; TCV, 19%; WDPTC, 23%; and widely invasive HCC, 7%. A differing histology between the primary tumor and metastasis was observed in 37% of cases (n = 16 patients). In the majority of instances (63%; 10 of 16 patients) this was noted as transformation to a higher grade. Of the primary tumors classified as PTC, 70% progressed to more aggressive histotypes in the metastasis. Tumor necrosis and extensive extrathyroid extension in the primary tumor were found to be independent predictors of poorer DSS in this group of patients (P = .015). Approximately 68% of the PDTC primary tumors were initially classified by the primary pathologist as better‐differentiated tumors on the basis of the presence of papillary and/or follicular architecture or the presence of typical PTC nuclear features.CONCLUSIONS.Several observations can be made based on the results of the current study. The majority of metastases in patients with RAIR PET‐positive metastases are of a histologically aggressive subtype. However, well‒differentiated RAIR metastatic disease is observable. Poorly differentiated disease is underrecognized in many cases if defined by architectural and nuclear features alone. The presence of tumor necrosis was found to be a strong predictor of aggressive behavior, even within this group of clinically aggressive tumors. Finally, there is a significant amount of histologic plasticity between primary tumors and metastases that may reflect the genetic instability of these tumors. Cancer 2008. © 2008 American Cancer Society.

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Section: Discussionmentioning

confidence: 99%

Histopathologic characterization of radioactive iodine‐refractory fluorodeoxyglucose‐positron emission tomography‐positive thyroid carcinoma

Rivera

Ghossein

Schöder

et al. 2008

Cancer

Self Cite

191

130

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“…Compared to well-differentiated carcinomas, anaplastic thyroid carcinomas are more likely to be aneuploid, 5 they demonstrate a much higher prevalence of loss of heterozygosity, 1,6 and they harbor alterations of key regulators of cell growth and differentiation that are not targeted in earlier stages of tumorigenesis. 7,8 As one example, mutations of p53 are commonly noted in anaplastic thyroid carcinomas, but they are rarely present in well-differentiated thyroid carcinomas. [9][10][11][12] BRAF encodes a serine-threonine kinase that acts in the mitogen activated protein kinase (MAPK) pathway.…”

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confidence: 99%

BRAF mutations in anaplastic thyroid carcinoma: implications for tumor origin, diagnosis and treatment

et al. 2004

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Anaplastic thyroid carcinoma is a highly aggressive neoplasm. Affected patients typically present with advanced disease where there is little hope for cure using conventional therapeutic modalities. Understanding the genetic alterations underlying the development of anaplastic thyroid carcinoma, such as mutational activation of BRAF, could help clarify its relationship with well-differentiated forms of thyroid carcinoma (ie follicular and papillary carcinoma) and could help select patients most likely to benefit from novel therapeutic strategies targeting BRAF. We tested 16 anaplastic thyroid carcinomas for the thymine (T)-adenine (A) missense mutation at nucleotide 1796 in the BRAF gene using a newly developed assay that employs a novel primer extension method (Mutector s assay). Seven of these anaplastic thyroid carcinomas arose in association with a well-differentiated thyroid carcinoma, and these were also evaluated. The 1796T-A mutation was detected in eight (50%) of the anaplastic thyroid carcinomas, in four of five (80%) associated papillary thyroid carcinomas, and in zero of two (0%) associated follicular carcinomas. In all seven cases where anaplastic thyroid carcinoma arose in association with a well-differentiated thyroid carcinoma, BRAF status in the two components was concordant. Like papillary thyroid carcinoma, a significant percentage of anaplastic thyroid carcinomas also harbor BRAF mutations. Indeed, when papillary thyroid carcinoma and anaplastic thyroid carcinoma occur together, they consistently share the same BRAF profile, supporting the notion that many anaplastic thyroid carcinomas actually represent progressive malignant degeneration of a pre-existing welldifferentiated thyroid carcinoma. The high frequency of BRAF mutations in a tumor that is generally regarded as uniformly fatal justifies evaluation of the potential benefits of anti-BRAF therapy for patients with anaplastic thyroid carcinoma.

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“…Molecular and immunohistochemical studies directed to detect specific gene profiles and related proteins in thyroid cancer have been extensively reported in literature (Bartolazzi et al, 2001;Huang et al, 2001;Ruco et al, 2001;Wreesmann et al, 2002). Experimental data, mostly arising from the molecular analysis of papillary thyroid carcinoma (PTC), contributed to identify a panel of genes overexpressed in thyroid malignancy.…”

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confidence: 99%

Detection and molecular characterisation of thyroid cancer precursor lesions in a specific subset of Hashimoto's thyroiditis

Gasbarri

Sciacchitano²,

Marasco

et al. 2004

Br J Cancer

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Hashimoto's thyroiditis (HT) represents the most common cause of hypothyroidism and nonendemic goiter, but its clinical and pathological heterogeneity opens the question if this disease should be more properly considered as a spectrum of different thyroid conditions rather than as a single nosological entity. In this study, we analysed 133 cases of HT for the expression of galectin-3, a lectin molecule involved in malignant transformation, apoptosis and cell cycle control. An unexpected expression of galectin-3 was demonstrated in a subset of HT together with the presence of HBME-1, c-met and cyclin-D1 that are also involved in malignant transformation and deregulated cell growth. Furthermore, a loss of allelic heterozygosity in a specific cancer-related chromosomal region was demonstrated in some HT harbouring galectin-3-positive follicular cells, by using laser capture microdissection. On the basis of the morphological and molecular findings we identified four subsets of HT: (a) HT with classic features of chronic autoimmune thyroiditis; (b) HT associated to hyperplastic/adenomatous lesions; (c) HT harbouring thyroid cancer precursors; (d) HT associated to unequivocal thyroid microcarcinomas. Our findings provide a well-substantiated morphological and molecular demonstration that HT may include a spectrum of different thyroid conditions ranging from chronic autoimmune thyroiditis to thyroiditis triggered by specific immune-response to cancer-related antigens.

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Genome-Wide Appraisal of Thyroid Cancer Progression

Cited by 155 publications

References 46 publications

Histopathologic characterization of radioactive iodine‐refractory fluorodeoxyglucose‐positron emission tomography‐positive thyroid carcinoma

Histopathologic characterization of radioactive iodine‐refractory fluorodeoxyglucose‐positron emission tomography‐positive thyroid carcinoma

BRAF mutations in anaplastic thyroid carcinoma: implications for tumor origin, diagnosis and treatment

Detection and molecular characterisation of thyroid cancer precursor lesions in a specific subset of Hashimoto's thyroiditis

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