4.3 Article

The impact of mitochondria-related POLG and TFAM variants on breast cancer pathomorphological characteristics and patient outcomes

Journal

BIOMARKERS
Volume 26, Issue 4, Pages 343-353

Publisher

TAYLOR & FRANCIS LTD
DOI: 10.1080/1354750X.2021.1900397

Keywords

TFAM; POLG; SNV; breast cancer; tumour phenotype; outcome

Funding

  1. Lithuanian University of Health Sciences

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This study investigated the association between single nucleotide variants in POLG and TFAM genes and tumour phenotype and disease outcome in breast cancer patients. Specific genotypes of POLG rs2307441 and rs2072267, as well as TFAM rs3900887, were found to be significantly associated with different tumour characteristics.
Purpose Breast cancer is the most frequent female cancer, leading to relapse with distant metastasis of approximately one-third of patients. Cancer is usually considered a genetic disease involving mutations in nuclear DNA. However, genes, coding for mitochondrial proteins or regulatory molecules, are rarely under consideration. This study aimed to analyse 10 single nucleotide variants in POLG and TFAM genes and assess their association with tumour phenotype and disease outcome. Materials and methods A total of 234 breast cancer patients were included in this study. Variations were determined with Real-Time PCR using TaqMan(R) probes. Results We found that patients with POLG rs2307441 TT and CT genotypes had a lower probability for vascular invasion than those with CC genotype (p = 0.001). Patients with POLG rs2072267 AG genotype were predisposed for progression compared with GG genotype (p = 0.015). TFAM rs3900887 TT genotype was associated with a higher probability for positive oestrogen receptors (p = 0.003) and lymphatic invasion (p = 0.001) in comparison to AA genotype, patients with TT (p = 0.000) were more likely to have positive lymph nodes. Conclusions Our data suggest that variations in POLG and TFAM genes are important determinacies of tumour phenotype and disease outcome in breast cancer patients.

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