| Literature DB >> 28853721 |
Oriol Calvete1,2, Pablo Garcia-Pavia3,4,5, Fernando Domínguez3,4,6, Gaelle Bougeard7, Kristin Kunze8, Andreas Braeuninger8, Alex Teule9, Adriana Lasa10, Teresa Ramón Y Cajal11, Gemma Llort12, Victoria Fernández1, Conxi Lázaro13, Miguel Urioste2,14, Javier Benitez1,2.
Abstract
The POT1 protein binds and protects telomeres. Germline variants in the POT1 gene have recently been shown to be associated with risk of developing tumors in different tissues such as familial chronic lymphocytic leukemia, colorectal, glioma and melanoma tumors. Recently, we uncovered a variant in the POT1 gene (p.R117C) as causative of familial cardiac angiosarcomas (CAS) in Li-Fraumeni-like (LFL) syndrome families. Our in silico studies predicted that this protein had lost the ability to interact with TPP1 and single-stranded DNA. In vitro studies corroborated this prediction and showed that this lack of function leads to abnormally long telomeres. To better understand the POT1 gene and its role with tumorigenesis, we extended the study to LFL (with and without members affected with angiosarcomas (AS)) and sporadic AS and cardiac sarcomas. We found POT1 variants in the 20% of the families with members affected with AS and 10% of sporadic AS and sarcomas. In silico studies predicted that these new variants were damaging in the same manner as previously described for the POT1 p.R117C variants. The wide spectrum of variants in the POT1 gene leading to tumorigenesis in different tissues demonstrates its general importance. Study of the POT1 gene should be considered as routine diagnostic in these cancers.Entities:
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Year: 2017 PMID: 28853721 PMCID: PMC5643968 DOI: 10.1038/ejhg.2017.134
Source DB: PubMed Journal: Eur J Hum Genet ISSN: 1018-4813 Impact factor: 5.351