POLE and POLD1 screening in 155 patients with multiple polyps and early-onset colorectal cancer

被引:39
作者
Esteban-Jurado, Clara [1 ]
Gimenez-Zaragoza, David [2 ]
Munoz, Jenifer [1 ]
Franch-Exposito, Sebastia [1 ]
Alvarez-Barona, Miriam [3 ]
Ocana, Teresa [1 ]
Cuatrecasas, Miriam [4 ]
Carballal, Sabela [1 ]
Lopez-Ceron, Mara [1 ]
Marti-Solano, Maria [5 ]
Diaz-Gay, Marcos [1 ]
van Wezel, Tom [6 ]
Castells, Antoni [1 ]
Bujanda, Luis [7 ]
Balmana, Judith [8 ,9 ]
Gonzalo, Victoria [10 ]
Llort, Gemma [11 ]
Ruiz-Ponte, Clara [3 ]
Cubiella, Joaquin [12 ]
Balaguer, Francesc [1 ]
Aligue, Rosa [2 ]
Castellvi-Bel, Sergi [1 ]
机构
[1] Univ Barcelona, CIBEREHD, Inst Invest Biomed August Pi i Sunyer IDIBAPS, Gastroenterol Dept,Hosp Clin Barcelona, Barcelona, Catalonia, Spain
[2] Univ Barcelona, Inst Invest Biomed August Pi i Sunyer IDIBAPS, Sch Med, Biomed Sci Dept, Barcelona, Catalonia, Spain
[3] Univ Santiago de Compostela, Galician Publ Fdn Genom Med FPGMX, CIBERER, Genom Med Grp,Hosp Clin, Santiago De Compostela, Galicia, Spain
[4] Hosp Clin Barcelona, Biobanc Clin, IDIBAPS, Dept Pathol, Barcelona, Catalonia, Spain
[5] Philipps Univ Marburg, Dept Pharmaceut Chem, Marburg, Germany
[6] Leiden Univ, Med Ctr, Leiden, Netherlands
[7] Univ Basque Country, CIBEREHD, Gastroenterol Dept, UPV EHU,Hosp Donostia,Inst Biodonostia, San Sebastian, Spain
[8] Univ Hosp Vall dHebron, Med Oncol Dept, High Risk & Canc Prevent Unit, Barcelona, Spain
[9] Vall dHebron Inst Oncol, Barcelona, Spain
[10] Hosp Univ Mutua Terrassa, Gastroenterol Dept, Barcelona, Spain
[11] Corp Parc Tauli, Clin Oncol Dept, Barcelona, Spain
[12] Complexo Hosp Univ Ourense, Inst Invest Biomed Ourense Pontevedra & Vigo, Gastroenterol Dept, Orense, Spain
关键词
colorectal neoplasm; colorectal adenoma; genetic predisposition to disease; POLE; POLD1; DNA-POLYMERASE EPSILON; MISMATCH REPAIR; GERMLINE MUTATIONS; CARCINOMAS; VARIANTS; ADENOMAS; FAMILIES;
D O I
10.18632/oncotarget.15810
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Germline mutations in POLE and POLD1 have been shown to cause predisposition to colorectal multiple polyposis and a wide range of neoplasms, early-onset colorectal cancer being the most prevalent. In order to find additional mutations affecting the proofreading activity of these polymerases, we sequenced its exonuclease domain in 155 patients with multiple polyps or an early-onset colorectal cancer phenotype without alterations in the known hereditary colorectal cancer genes. Interestingly, none of the previously reported mutations in POLE and POLD1 were found. On the other hand, among the genetic variants detected, only two of them stood out as putative pathogenic in the POLE gene, c. 1359 + 46del71 and c. 1420G > A (p.Val474Ile). The first variant, detected in two families, was not proven to alter correct RNA splicing. Contrarily, c. 1420G > A (p. Val474Ile) was detected in one early-onset colorectal cancer patient and located right next to the exonuclease domain. The pathogenicity of this change was suggested by its rarity and bioinformatics predictions, and it was further indicated by functional assays in Schizosaccharomyces pombe. This is the first study to functionally analyze a POLE genetic variant outside the exonuclease domain and widens the spectrum of genetic changes in this DNA polymerase that could lead to colorectal cancer predisposition.
引用
收藏
页码:26732 / 26743
页数:12
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