Clinical Endocrinology

Volume 87, Issue 4
ORIGINAL ARTICLE

Identification of somatic TERT promoter mutations in familial nonmedullary thyroid carcinomas

Inês J. Marques

Unidade de Investigação em Patobiologia Molecular (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

Chronic Diseases Research Centre (CEDOC), Universidade Nova de Lisboa, Lisboa, Portugal

Nova Medical School/Faculdade de Ciências Médicas, Universidade Nova de Lisboa, Lisboa, Portugal

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Margarida M. Moura

Unidade de Investigação em Patobiologia Molecular (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

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Rafael Cabrera

Serviço de Anatomia Patológica, Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

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António E. Pinto

Serviço de Anatomia Patológica, Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

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Joana Simões‐Pereira

Unidade de Investigação em Patobiologia Molecular (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

Nova Medical School/Faculdade de Ciências Médicas, Universidade Nova de Lisboa, Lisboa, Portugal

Serviço de Endocrinologia, Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

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Catarina Santos

Serviço de Genética, Instituto Português de Oncologia do Porto Francisco Gentil, Porto, Portugal

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Francisco D. Menezes

Serviço de Anatomia Patológica, Instituto Português de Oncologia do Porto Francisco Gentil, Porto, Portugal

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Diana Montezuma

Serviço de Anatomia Patológica, Instituto Português de Oncologia do Porto Francisco Gentil, Porto, Portugal

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Rui Henrique

Serviço de Anatomia Patológica, Instituto Português de Oncologia do Porto Francisco Gentil, Porto, Portugal

Departamento de Patologia e Imunologia Molecular, Instituto de Ciências Biomédicas Abel Salazar, Universidade do Porto, Porto, Portugal

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Manuel Rodrigues Teixeira

Serviço de Genética, Instituto Português de Oncologia do Porto Francisco Gentil, Porto, Portugal

Departamento de Patologia e Imunologia Molecular, Instituto de Ciências Biomédicas Abel Salazar, Universidade do Porto, Porto, Portugal

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Valeriano Leite

Unidade de Investigação em Patobiologia Molecular (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

Nova Medical School/Faculdade de Ciências Médicas, Universidade Nova de Lisboa, Lisboa, Portugal

Serviço de Endocrinologia, Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

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Branca M. Cavaco

Corresponding Author

E-mail address: bcavaco@ipolisboa.min-saude.pt

Unidade de Investigação em Patobiologia Molecular (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal

Correspondence

Branca M. Cavaco, Unidade de Investigação em Patobiologia Molecular, Instituto Português de Oncologia de Lisboa Francisco Gentil, Lisboa, Portugal.

Email: bcavaco@ipolisboa.min-saude.pt

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First published: 14 May 2017
https://doi.org/10.1111/cen.13375
Cited by: 3

Summary

Objective

The genes causing familial nonmedullary thyroid carcinoma (FNMTC) identified to date are only involved in a small fraction of the families. Recently, somatic mutations in TERT promoter region and in EIF1AX gene were reported in thyroid tumours of undefined familial status. The aim of this study was to investigate the role of TERT and EIF1AX mutations in familial thyroid tumours.

Design

The promoter region of TERT was sequenced in leucocyte DNA of the probands from 75 FNMTC families. In thyroid tumours from 54 familial cases, we assessed somatic TERT promoter, RAS and BRAF hotspot mutations, and the whole EIF1AX gene.

Results

No potentially pathogenic germline variants were identified in TERT in the 75 FNMTC families’ probands. In the 54 carcinomas, we identified five cases (9%) with hotspot somatic TERT promoter mutations. BRAF mutations were found in 41% of the tumours. All TERT‐positive samples were also positive for BRAF p.Val600Glu, and this co‐occurrence was found to be statistically significant (P=.008). RAS mutations were detected in four tumours wild‐type for TERT (7%). Evaluation of tumour mutation data together with the patients’ clinicopathological features revealed a significant correlation between TERT plus BRAF mutations and advanced tumour stage (T4) (P=.020). No mutations were identified in EIF1AX.

Conclusions

The results of this study suggest that TERT promoter and EIF1AX mutations are not frequently involved in FNMTC aetiology. However, we show for the first time that TERT alterations are associated with familial thyroid tumour progression. Our data also suggest that TERT mutations are more often found in concomitance with BRAF mutations in advanced stages of FNMTC.

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