Development of metastatic poorly differentiated thyroid cancer from a sub-centimeter papillary thyroid carcinoma in a young patient with a germline MET mutation \u2013 association or random chance?

Klara Johansson,Jan Zedenius,Adam Stenman,C Christofer Juhlin,Na Wang,Johan O Paulsson,Catharina Ihre-Lundgren

doi:10.1186/s13044-021-00110-4

Abstract

BackgroundThyroid cancer dedifferentiation is an unusual observation among young patients and is poorly understood, although a recent correlation to DICER1 gene mutations has been proposed.Case presentationA 28-year old patient presented with a sub-centimeter cytology-verified primary papillary thyroid carcinoma (PTC) and a synchronous lateral lymph node metastasis. Following surgery, histopathology confirmed a 9 mm oxyphilic PTC and a synchronous metastasis of poorly differentiated thyroid carcinoma (PDTC). Extensive molecular examinations of both lesions revealed wildtype DICER1 sequences, but identified a somatic ETV6-NTRK3 gene fusion and a MET germline variant (c.1076G > A, p.Arg359Gln). MET is an established oncogene known to be overexpressed in thyroid cancer, and this specific alteration was not reported as a single nucleotide polymorphism (SNP), suggestive of a mutation. Both the primary PTC and the metastatic PDTC displayed strong MET immunoreactivity. A validation cohort of 50 PTCs from young patients were analyzed using quantitative real-time PCR, revealing significantly higher MET gene expression in tumors than normal thyroid controls, a finding which was particularly pronounced in BRAF V600E mutated cases. No additional tumors apart from the index case harbored the p.Arg359Gln MET mutation. Transfecting PTC cell lines MDA-T32 and MDA-T41 with a p.Arg359Gln MET plasmid construct revealed no obvious effects on cellular migratory or invasive properties, whereas overexpression of wildtype MET stimulated invasion.ConclusionsThe question of whether the observed MET mutation in any way influenced the dedifferentiation of a primary PTC into a PDTC metastasis remains to be established. Moreover, our data corroborate earlier studies, indicating that MET is aberrantly expressed in PTC and may influence the invasive behavior of these tumors.

Highlights

Thyroid cancer dedifferentiation is an unusual observation among young patients and is poorly under‐ stood, a recent correlation to DICER1 gene mutations has been proposed.Case presentation: A 28-year old patient presented with a sub-centimeter cytology-verified primary papillary thy‐ roid carcinoma (PTC) and a synchronous lateral lymph node metastasis
The question of whether the observed MET protooncogene (MET) mutation in any way influenced the dedifferentiation of a primary PTC into a poorly differentiated thyroid carcinoma (PDTC) metastasis remains to be established
Our data corroborate earlier studies, indicat‐ ing that MET is aberrantly expressed in PTC and may influence the invasive behavior of these tumors

Summary

Conclusions

The question of whether the observed MET mutation in any way influenced the dedifferentiation of a primary PTC into a PDTC metastasis remains to be established.

Findings

Background

Discussion and conclusions