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Endocrine Abstracts (2023) 92 OP12-01 | DOI: 10.1530/endoabs.92.OP-12-01

ETA2023 45th Annual Meeting of the European Thyroid Association ETA 2023 Oral Session 12: Emerging Insights into Thyroid Cancer Genetics (5 abstracts)

Prospective evaluation of thyrospec molecular testing of indeterminate thyroid nodule cytologies following diagnostic pathway optimization

Paul Stewardson 1 , Markus Eszlinger 2 , Jiahui Wu 3 , Moosa Khalil 4 , Douglas J Demetrick 5 , Winson Cheung 6 , Adrian Box 4 & Ralf Paschke 7


1University of Calgary, University of Calgary, Department of Medical Science, Calgary, Canada; 2Institute of Pathology, Molecular Pathology, Cumming School of Medicine, Halle (Saale), Germany; 3University of Calgary, Arnie Charbonneau Cancer Institute, Cumming School of Medicine, Calgary, Canada; 4University of Calgary, Cumming School of Medicine, Department of Pathology and Laboratory Medicine, Calgary, Ab, Canada; 5Pathology and Laboratory Medicine, Cumming School of Medicine, Calgary, Canada; 6Cumming School of Medicine, Oncology, Calgary, Canada; 7Department of Medicine, Cumming School of Medicine, University of Calgary, Calgary, Canada


Objectives: Molecular diagnostic tests for indeterminate thyroid nodules (ITNs) are marketed based on negative predictive value (NPV) and benign call rate. Arguments that unnecessary surgeries are avoided based on NPV/BCR incorrectly assume that all ITNs would undergo diagnostic surgery in the absence of molecular testing. In our practice with centralized triage and cytopathology the resection and malignancy rate, respectively, were 21% and 26% for AUS/FLUS and 56% and 43% for FN/SFN, prior to molecular testing implementation. If each positive molecular test result triggered surgery, implementation of molecular testing would substantially increase overtreatment. Therefore, following optimization of ultrasound malignancy risk assessment (Wu et al ETJ 2022) and evaluation of local malignancy rates (Ghaznavi et al Acta Cytologica 2022) in each Bethesda cytologic category for our diagnostic pathway, we locally developed and validated ThyroSPEC, a low-cost (C=650) molecular diagnostic test that detects 117 point mutations and 23 gene fusions in residual routine FNA material.

Methods: We followed 615 consecutive patients with ITN from July 2020 to July 2022 with reflex ThyroSPEC testing in the context of a centralized, optimized thyroid nodule diagnostic pathway to determine the strengths and gaps of this integrated diagnostic pathway.

Results: The resection rate for ITNs was 217/615 (35%) with molecular testing at a 59/143 (41%) prevalence of malignancy in AUS/FLUS and 21/41 (51%) prevalence of malignancy in FN/SFN, a relative increase of 13% (P = 0.0913) in the resection rate and 15% (P = 0.2438) in the malignancy rate since implementation of ThyroSPEC.

Table 1: ThyroSPEC performance stratified by ultrasound malignancy risk categories. Ranges are from resected nodules only (n =52,71,32) to all resected nodules plus unresected nodules with more than 1 year follow up (n =88,161,78).
CytologynSensitivitySpecificityNPVPPV
ATA Low Suspicion, TR352-8872%56-83%79-92%46-52%
ATA Intermediate Suspicion, TR471-16180%69-79%78-93%52-72%
ATA High Suspicion, TR532-7846%83-84%70-89%35-67%
The primary reason for surgery in ThyroSPEC positive and negative ITNs was mutation status 78/103 (76%) and ultrasound or cytology risk categories 38/106 (36%), respectively. RAS mutations had a 22% prevalence and 58% malignancy rate, therefore resecting all RAS positives would induce overtreatment.

Conclusions: This ongoing study involved first optimizing the local ultrasound and cytology practices as major factors in decision-making, then implementing a custom molecular test into a low resection rate thyroid nodule diagnostic pathway. This resulted in improved decision-making and higher diagnostic yield particularly for diagnostically difficult ultrasound intermediate suspicion nodules.

Volume 92

45th Annual Meeting of the European Thyroid Association (ETA) 2023

European Thyroid Association 

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