Abstract
BackgroundThe molecular etiology of thyroid carcinoma (TC) and other thyroid diseases which may present malignant precursor lesions is not fully explored yet. The purpose of this study was to estimate frequency, type and clinicopathological value of BRAF exon 15 mutations in different types of cancerous and non-cancerous thyroid lesions originating in an ethnically diverse population.MethodsBRAF exon 15 was sequenced in 381 cases of thyroid lesions including Hashimoto´s thyroiditis, nodular goiters, hyperplastic nodules, follicular adenomas (FA), papillary TC (PTC), follicular variant PTC (FVPTC), microcarcinomas of PTC (micro PTC; tumor size ≤ 1 cm), follicular TC (FTC), and non-well differentiated TC (non-WDTC).ResultsWe identified BRAF mutations in one of 69 FA, 72 of 115 (63%) PTC, seven of 42 (17%) FVPTC, 10 of 56 (18%) micro PTC, one of 17 (6%) FTC, and one of eight (13%) non-WDTC. Most of the cases showed the common V600E mutation. One case each of PTC, FVPTC, and FTC harbored a K601E mutation. A novel BRAF mutation was identified in a FA leading to deletion of threonine at codon 599 (p.T599del). A rare 3-base pair insertion was detected in a stage III PTC resulting in duplication of threonine at codon 599 (p.T599dup). Patients with PTC harboring no BRAF mutation (BRAFwt) were on average younger than those with a BRAF mutation (BRAFmut) in the PTC (36.6 years vs. 43.8 years). Older age (≥ 45 years) in patients with PTC was significantly associated with tumor size ≥ 4 cm (P = 0.018), vessel invasion (P = 0.004), and distant metastasis (P = 0.001). Lymph node (LN) involvement in PTC significantly correlated with tumor size (P = 0.044), and vessel invasion (P = 0.013). Of notice, taken the whole TC group, family history of thyroid disease positively correlated with capsular invasion (P = 0.025).ConclusionsOlder age is manifold associated with unfavorable tumor markers in our series. The K601E identified in a PTC, FVPTC, and FTC seems to be more distributed among different histological types of TC than previously thought. The T599del is a yet undescribed mutation and the rare T599dup has not been reported as a mutation in PTC so far.
Highlights
The molecular etiology of thyroid carcinoma (TC) and other thyroid diseases which may present malignant precursor lesions is not fully explored yet
With the exception of Medullary TC (MTC) [13] the most common, surgically treated thyroid diseases were included in the study, i.e. Hashimotos thyroiditis, nodular goiters, hyperplastic lesions, follicular adenomas (FA), follicular TC (FTC), papillary TC (PTC) (> 1 cm), follicular variant PTC (FVPTC) (> 1 cm), micro PTC (≤ 1 cm) and non-well differentiated TC, The non-WDTC group comprised poorly differentiated insular variant PTC, combinatorial PTC/ Anaplastic TC (ATC), and ATC
Almost all micro PTC were classified as stage I tumors except two multifocal stage III tumors and one stage IV tumor (Table 2)
Summary
The molecular etiology of thyroid carcinoma (TC) and other thyroid diseases which may present malignant precursor lesions is not fully explored yet. Median age of women diagnosed with TC in Saudi Arabia is considerable lower than for men (37 years vs 43 years). Females in this country are more commonly diagnosed with FVPTC (19.3% vs 9.6%) and micro PTC (7.4% vs 2.6%) than males. PTC represents about 80% of differentiated TC with an increasing trend while FTC (~11%), Hurthle cell carcinoma (~3%), MTC (~4%), and ATC (~2%) represent minor variants [2]. A study on the pattern of TC arising in Jeddah, an ethnically diverse metropolis in Western Saudi Arabia, revealed a common distribution of histological types: PTC (82%), FTC (4.4%), ATC (6.7%), and MTC (6.7%) [5]
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