The genetic landscape of benign thyroid nodules revealed by whole exome and transcriptome sequencing

The genomic alterations for benign thyroid nodule, especially adenomatoid nodule, one of the most common types of hyperplasia lesion, are ill-studied. Here, we show whole-exome sequencing and/or transcriptome sequencing data on adenomatoid nodules with or without coincidental papillary thyroid carci...

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Veröffentlicht in:Nature communications 2017-06, Vol.8 (1), p.15533-15533, Article 15533
Hauptverfasser: Ye, Lei, Zhou, Xiaoyi, Huang, Fengjiao, Wang, Weixi, Qi, Yicheng, Xu, Heng, Shu, Yang, Shen, Liyun, Fei, Xiaochun, Xie, Jing, Cao, Min, Zhou, Yulin, Zhu, Wei, Wang, Shu, Ning, Guang, Wang, Weiqing
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Sprache:eng
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Zusammenfassung:The genomic alterations for benign thyroid nodule, especially adenomatoid nodule, one of the most common types of hyperplasia lesion, are ill-studied. Here, we show whole-exome sequencing and/or transcriptome sequencing data on adenomatoid nodules with or without coincidental papillary thyroid carcinoma (PTC). Somatic mutation of BRAF (22/32) is only detected in PTC, while mutations in SPOP (4/38), ZNF148 (6/38) and EZH1 (3/38) are found enriched in adenomatoid nodule. In an expanded cohort of adenomatoid nodule ( n =259) mutually exclusive SPOP P94R , EZH1 Q571R and ZNF148 mutations are identified in 24.3% of them. Adenomatoid nodules show very few overlapped mutations and distinct gene expression patterns with their coincidental PTC. Phylogenetic tree analysis uncovers that PTCs evolved independently from their matched benign nodules. Our findings reveal that benign nodules possess a unique molecular signature that differs from PTC and provide genomic evidence for the conventional belief that PTC and benign nodules have independent origin. Papillary thyroid carcinomas are often found with coincidental benign thyroid nodules. Here, the authors provide genomic evidence that papillary thyroid carcinomas and coincidental benign thyroid nodules originate and evolve independently.
ISSN:2041-1723
2041-1723
DOI:10.1038/ncomms15533