The impact of noninvasive follicular thyroid neoplasm with papillary‐like nuclear features on the performance of the Afirma gene expression classifier

Hang, Jen‐Fan; Westra, William H.; Cooper, David S.; Ali, Syed Z.

doi:10.1002/cncy.21879

Cited by 58 publications

(66 citation statements)

References 41 publications

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“…Two of these cases had undergone preoperative molecular testing, both with GEC Suspicious results. The current use of NIFTP nomenclature appears to lower the positive predictive value (PPV) as previously published by Hang et al; they observed a reduction in PPV to identify malignancy from 23% to 13% in the FN/SFN group. Recent publication from Jug et al also noted a reduction in PPV for both the Afirma GEC and ThyroSeq v2 when accounting for nonmalignant NIFTP lesions, from 30.1% to 25.3% and 42.9% to 14.3%, respectively.…”

Section: Discussionmentioning

confidence: 52%

Outcomes of Bethesda categories III and IV thyroid nodules over 5 years and performance of the Afirma gene expression classifier: A single‐institution study

Deaver

Haugen

Pozdeyev

et al. 2018

Clinical Endocrinology

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Section: Discussionmentioning

confidence: 52%

Outcomes of Bethesda categories III and IV thyroid nodules over 5 years and performance of the Afirma gene expression classifier: A single‐institution study

Deaver

Haugen

Pozdeyev

et al. 2018

Clinical Endocrinology

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“…The initial prospective validated GEC study did not consider NIFTP, and only few papers have evaluated the impact of NIFTP on the performance of GEC. The diagnostic role of the Afirma test to detect NIFTP has been controversial . As reported in different series, NIFTP is associated with suspicious Afirma GEC results .…”

Section: Niftp and Molecular Testingmentioning

confidence: 98%

“…This recent acknowledgement of the role of molecular testing formalizes their use in defining risk stratification of patients with thyroid nodules. In this review, we discuss the clinical implications of the different molecular tests in the indeterminate Bethesda categories . It is important to note that the literature to date generally supports employing a combination of morphology and molecular testing to best guide the clinical or surgical approach for patients diagnosed with indeterminate thyroid nodules (Table ).…”

Section: Molecular Test Options and Molecular Approach To Indeterminamentioning

confidence: 99%

“…Wong et al reported that the Afirma GEC is a useful aid to detect NIFTP and that many of the carcinomas detected by Afirma are in fact noninvasive FVPTCs. Hang et al evaluated the impact of the introduction of NIFTP on the performance of the Afirma GEC. The investigators studied 384 indeterminate thyroid nodules (including AUS/FLUS and SFN/FN) where 177 had surgical follow‐up.…”

Section: Niftp and Molecular Testingmentioning

confidence: 99%

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Ancillary molecular testing of indeterminate thyroid nodules

Rossi

Larocca

Pantanowitz

2018

Cancer Cytopathology

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Cytological specimens from thyroid nodules are increasingly being adopted as the first available material for cost effectively managing patients in the era of personalized medicine. Cytology aspirates not only play a central role in providing accurate diagnoses, but are also being collected for ancillary molecular testing. Molecular analysis, including the evaluation of somatic mutations and other genomic alterations, has accordingly become well integrated in the cytological workup of thyroid lesions. Appropriately handled thyroid cytology preparations provide well-preserved and adequately cellular material with improved DNA/RNA quantity. The recent publication of the 2nd edition of The Bethesda System for Reporting Thyroid Cytopathology and the American Thyroid Association guidelines confirm the relevant role of molecular testing in the management of the different subcategories of indeterminate thyroid lesions. This review discusses the role of molecular testing for indeterminate thyroid nodules, including the recent introduction of the noninvasive, encapsulated follicular variant of papillary thyroid carcinoma (FVPTC), known also as noninvasive follicular neoplasm with papillary-like nuclear features (NIFTP).

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“…Hang et al suggested that separating lesions with and without Hurthle cell features may be helpful to maximize the benefit of Afirma GEC in the latter group 19. Hang et al suggested that separating lesions with and without Hurthle cell features may be helpful to maximize the benefit of Afirma GEC in the latter group 19.…”

mentioning

confidence: 99%

Hurthle cell predominance impacts results of Afirma gene expression classifier and ThyroSeq molecular panel performance in indeterminate thyroid nodules

Parajuli

Jug

Ahmadi

et al. 2019

Diagnostic Cytopathology

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Background: Molecular tests such as the Afirma gene expression classifier (GEC) and mutational panels (such as ThyroSeq) have been introduced to help risk stratify cytologically indeterminate thyroid nodules with the aim to reduce the number of unnecessary thyroidectomies. Some reports have suggested that samples with Hurthle cell predominance have higher false-positive rates on GEC testing, but data are limited. Methods:We reviewed thyroid nodules with indeterminate (Bethesda III/IV) cytology at our institution. Patient demographics, cytologic and histologic diagnoses (where available), and molecular test results were collected.Results: GEC was performed on 202 nodules, and ThyroSeq was performed on 81 nodules. In the GEC cohort, 66% of nodules with Hurthle cell predominance yielded "suspicious" result vs 46% of nodules without Hurthle cell predominance, with risk of malignancy (ROM) for surgically resected nodules of 16% and 33%, respectively. In ThyroSeq cohort, 8% of nodules with Hurthle cell predominance yielded a high-risk mutation vs 19% of nodules without Hurthle cell predominance, with ROM of 50% and 33%, respectively.Conclusions: For ThyroSeq molecular panel, while it did not appear that there was an increase in rate of high-risk mutations detected in the samples with Hurthle cell predominance, small numbers limit the generalizability of these results. For the GEC cohort, indeterminate thyroid nodules with predominance of Hurthle cells showed an increased rate of "suspicious" results compared to samples without Hurthle cell predominance. The ROM for GEC "suspicious" nodules with Hurthle cell predominance on surgical resection was lower in our study. Repeat FNA may be of use in patients with these types of nodules. In the context of a Hurthle cell predominant lesion, positive results on molecular testing may not carry a high rate of malignancy.

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The impact of noninvasive follicular thyroid neoplasm with papillary‐like nuclear features on the performance of the Afirma gene expression classifier

Cited by 58 publications

References 41 publications

Outcomes of Bethesda categories III and IV thyroid nodules over 5 years and performance of the Afirma gene expression classifier: A single‐institution study

Outcomes of Bethesda categories III and IV thyroid nodules over 5 years and performance of the Afirma gene expression classifier: A single‐institution study

Ancillary molecular testing of indeterminate thyroid nodules

Hurthle cell predominance impacts results of Afirma gene expression classifier and ThyroSeq molecular panel performance in indeterminate thyroid nodules

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