Discovery of recessive effect of human polymerase δ proofreading deficiency through mutational analysis of POLD1-mutated normal and cancer cells.
Maria A AndrianovaVladimir B SeplyarskiyMariona TerradasAna Beatriz Sanchez-HerasPilar MurJosé Luís SotoGemma AizaEmma BorràsFyodor A KondrashovAlexey S KondrashovGeorgii A BazykinLaura VallePublished in: European journal of human genetics : EJHG (2024)
Constitutional heterozygous pathogenic variants in the exonuclease domain of POLE and POLD1, which affect the proofreading activity of the corresponding polymerases, cause a cancer predisposition syndrome characterized by increased risk of gastrointestinal polyposis, colorectal cancer, endometrial cancer and other tumor types. The generally accepted explanation for the connection between the disruption of the proofreading activity of polymerases epsilon and delta and cancer development is through an increase in the somatic mutation rate. Here we studied an extended family with multiple members heterozygous for the pathogenic POLD1 variant c.1421T>C p.(Leu474Pro), which segregates with the polyposis and cancer phenotypes. Through the analysis of mutational patterns of patient-derived fibroblasts colonies and de novo mutations obtained by parent-offspring comparisons, we concluded that heterozygous POLD1 L474P just subtly increases the somatic and germline mutation burden. In contrast, tumors developed in individuals with a heterozygous mutation in the exonuclease domain of POLD1, including L474P, have an extremely high mutation rate (>100 mut/Mb) associated with signature SBS10d. We solved this contradiction through the observation that tumorigenesis involves somatic inactivation of the wildtype POLD1 allele. These results imply that exonuclease deficiency of polymerase delta has a recessive effect on mutation rate.
Keyphrases
- papillary thyroid
- endometrial cancer
- early onset
- copy number
- squamous cell
- endothelial cells
- magnetic resonance
- type diabetes
- magnetic resonance imaging
- intellectual disability
- gene expression
- squamous cell carcinoma
- high throughput
- dna methylation
- computed tomography
- metabolic syndrome
- high fat diet
- autism spectrum disorder
- anti inflammatory
- childhood cancer
- genome wide
- dna damage
- pluripotent stem cells