Abstract 2225P
Background
Transcription factors play a critical role in tissue homeostasis and development and can also have roles in carcinogenesis. The aim of the study was to perform the genomyc analysis of the Forkhead box protein E1 gene (FOXE1) and NK2 homeobox 1 gene (NKX2-1) mutations in patients with Papillary thyroid cancer (PTC) and healthy control group as well as to compare the obtained results with clinical findings.
Methods
The study included 112 patients diagnosed with PTC (classical, tall cell and follicular variant) (aged 41-74 years) as well as 124 healthy controls (aged 29-80 years). Mutations of the FOX1 gene (rs965513) and NKX2-1 gene (rs944289) were detected using Real-time polymerase chain reaction method. Diagnosis of PTC was confirmed with cyto/histopathological examination.
Results
The genomyc analysis for FOX1 (rs965513) showed that the genotypes “AA,” “AG,” and minor allele “A” were more frequent in patients with PTC than in healthy control group (PTC p(genotype)=0.00071; p(allele)=0.004 vs. PTC p(genotype)=0.23; p(allele)=0.03). A further subsequent analysis of the PTC patients stratified for primary tumor stage (T1-T4), the absence/ presence of regional lymph node metastases (N0/N1) as well for distant metastases (M0/M1), showed an association of FOX1 (rs965513) with stages T1-T3 and N1. We could not find an association between the the NKX2-1 gene mutational status (rs944289) and the development of PTC. Additional analysis based on the BRAF mutational status showed strong correlation of FOX1 (rs965513) with BRAFV600E(+) cases (p=0.0001), but not with BRAFV600E(-) cases (p=0.123). For NKX2-1 (rs944289), both subgroups showed no correlation (p=0.04987 for BRAFV600E(+) cases; p=0.0463 for BRAFV600E(-) cases).
Conclusions
The results of our study show that the FOXE1 (rs965513) carry an increased risk for PTC development, particularly allele “A” and the genotypes “AA” and “AG” as well as developing of advanced PTC, which may reflect the course of a more aggressive disease. The NKX2-1 (rs944289) appears to play a non significant role in development of PTC.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
2326P - Circulating tumor DNA (ctDNA) dynamics and clinical outcome in metastatic colorectal cancer (mCRC) patients (pts) undergoing front-line chemotherapy
Presenter: Michele Ghidini
Session: Poster session 16
2327P - The impact of the microenvironment on the intratumoral cellular heterogeneity in colorectal cancer
Presenter: Idan Carmi
Session: Poster session 16
2328P - Alternative molecular mechanisms underpinning breast invasive lobular carcinoma identified by genomics-driven artificial intelligence model
Presenter: Fresia Pareja
Session: Poster session 16
2329P - Evidence for the utility of artificial intelligence and image analysis in Ki-67 quantification in solid tumors
Presenter: Xavier Pichon
Session: Poster session 16
2331P - Interest of next generation sequencing (NGS) for integrated molecular diagnosis of HER2-low breast cancer
Presenter: Jean Louis Merlin
Session: Poster session 16
2332P - Overall survival in breast cancer patients with HER2-low status single- center experience
Presenter: Joanna Huszno
Session: Poster session 16
2333P - Associating BRCA1 hypermethylation with clinicopathological and molecular variables in triple-negative breast cancers
Presenter: Anna Karlsson
Session: Poster session 16
2334P - Pathologic patterns following different neoadjuvant therapies in non-small cell lung cancer (NSCLC)
Presenter: Annikka Weissferdt
Session: Poster session 16
2335P - Spatial whole exome sequencing reveals the genetic features of highly-aggressive components in lung adenocarcinoma
Presenter: Jianfu Li
Session: Poster session 16