2018
DOI: 10.1002/dc.24091
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Determining the molecular test for indeterminate thyroid nodules best suited for our practice: A quality assurance study

Abstract: IntroductionCurrently, molecular studies are widely used as a guiding tool in further management of cytologically indeterminate thyroid nodules. At our institution, clinicians have recently expressed concern over receiving “less positive molecular results” upon switching from an extended 14 gene mutation panel (EGMP) to a 7 gene mutation panel (GMP). Our goal is to compare outcomes of these two tests in regards to the performance characteristics and clinical impact.Materials and MethodsAll thyroid fine‐needle … Show more

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Cited by 5 publications
(6 citation statements)
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“…{ Nodules from certain publications (33)(34)(35)(36)38) were tested by 7-or 14-gene panels but only reported data on a subset of genes, variants, and/or fusions. x One publication (37) analyzed nodules and reported data on two different panels.…”
Section: Inclusion/exclusion Criteriamentioning
confidence: 99%
See 2 more Smart Citations
“…{ Nodules from certain publications (33)(34)(35)(36)38) were tested by 7-or 14-gene panels but only reported data on a subset of genes, variants, and/or fusions. x One publication (37) analyzed nodules and reported data on two different panels.…”
Section: Inclusion/exclusion Criteriamentioning
confidence: 99%
“…Only 5 of 36 reported variants were reported with this frequency. a Although one study (37) specifically referred to mutation in MET, panel did not mention MET as a gene being analyzed for variants. The other study (56) did not say how MET was affected, only that it was positive.…”
Section: Figmentioning
confidence: 99%
See 1 more Smart Citation
“…Some gene variants including TP53, TERT and TERT gene fusions (indicated with * in Figure 1) are rather not specific for a follicular lesion per se, and may be found in various types of thyroid lesion, so, on its own, may justify the modification of a Bethesda III to Bethesda V. GLIS gene fusions are associated with hyalinizing trabecular tumours and may modify the Bethesda class as Bethesda V. Concurrent EIF1AX and RAS variants are reported to occur in advanced thyroid carcinomas promoting tumorigenesis 51 ; however, also NIFTP cases have been described harbouring concurrent EIF1AX and RAS variants. 44,52 TERT promoter variants, concurrent TERT and RAS variants or TERT and BRAF V600E gene variants are also reported to indicate a more aggressive nature with worse prognosis. [53][54][55][56][57] In case of GLIS translocations (modification to Bethesda V), a lobectomy is the appropriate treatment, for this translocation is highly specific for hyalinizing trabecular tumour (a benign lesion).…”
Section: Current Evidence In the Literature And Interpretation Of Molecular Diagnostic Resultsmentioning
confidence: 99%
“…These molecular alterations, also see Figure 1, as being mostly associated with follicular lesions and may occur in follicular adenoma/NIFTP/FVPTC/FTC, would hence suit Bethesda IV. Some gene variants including TP53 , TERT and TERT gene fusions (indicated with * in Figure 1) are rather not specific for a follicular lesion per se, and may be found in various types of thyroid lesion, so, on its own, may justify the modification of a Bethesda III to Bethesda V. GLIS gene fusions are associated with hyalinizing trabecular tumours and may modify the Bethesda class as Bethesda V. Concurrent EIF1AX and RAS variants are reported to occur in advanced thyroid carcinomas promoting tumorigenesis 51 ; however, also NIFTP cases have been described harbouring concurrent EIF1AX and RAS variants 44,52 . TERT promoter variants, concurrent TERT and RAS variants or TERT and BRAF V600E gene variants are also reported to indicate a more aggressive nature with worse prognosis 53–57 …”
Section: Introductionmentioning
confidence: 99%