Table 1.
Detailed listing of gene mutations associated with sporadic thyroid carcinomas
| Gene | Mutations | Activating or Inactivating | Common associations |
|---|---|---|---|
| AKT1 | G49A | Activating | Poorly differentiated carcinomas. |
| ALK | Exon 23 | Activating | Poorly differentiated and anaplastic carcinomas. |
| BRAF | V600E, K601E, AKAP9 gene fusion | Activating | Papillary and anaplastic carcinomas. V600E is by far most common and is over-represented in tall cell variant, uncommon in follicular variant. AKAP9-BRAF is over-represented in radiation induced papillary carcinomas. |
| CTNNB1 | Exon 3 | Activating | Poorly differentiated and anaplastic carcinomas. |
| IDH1 | Exon 4 | Abnormal activity | Identified in a minor fraction of most types of thyroid carcinoma. |
| NDUFA13 (GRIM19) | various | Inactivating | Hurthle cell carcinoma. |
| NTRK1 | Gene fusions with TPM3, TPR, and TFG | Activating | Infrequently found in papillary carcinoma. |
| PIK3CA | Exons 9, 20 | Activating | Follicular, poorly differentiated, and anaplastic carcinomas. |
| PPARG | Gene fusion with PAX8, rarely with CREB3L2 | Context dependent | Follicular carcinomas and follicular variant of papillary carcinomas. |
| PTEN | Deletion or inactivating mutation | Inactivating | Follicular, poorly differrentiated and anaplastic carcinomas. |
| RAS | NRAS Q61, HRAS Q61, KRAS G12, G13 | Activating | Follicular, follicular variant of papillary, poorly differentiated and anaplastic carcinomas. NRAS mutations are most common, KRAS are least common. |
| RET | Gene fusions with CCDC6 (RET/PTC1), NCOA4 (RET/PTC3), and others | Activating | Papillary carcinomas. Gene fusions result in constitutively active RET kinase domain. RET/PTC1 and RET/PTC3 are over-represented in radiation induced thyroid cancer. |
| TP53 | Exons 5–8 | Inactivating | Poorly differentiated and anaplastic carcinomas. |