Marabelli Monica, Molinaro Valeria, Abou Khouzam Raefa, Berrino Enrico, Panero Mara, Balsamo Antonella, Venesio Tiziana, Ranzani Guglielmina Nadia
1 Department of Biology and Biotechnology, University of Pavia , Pavia, Italy .
2 Candiolo Cancer Institute , FPO-IRCCS, Torino, Italy .
Genet Test Mol Biomarkers. 2016 Dec;20(12):777-785. doi: 10.1089/gtmb.2016.0198. Epub 2016 Oct 5.
Colorectal adenomatous polyposis entailing cancer predisposition is caused by constitutional mutations in different genes. APC is associated with the familial adenomatous polyposis (FAP/AFAP) and MUTYH with the MUTYH-associated polyposis (MAP), while POLE and POLD1 mutations cause the polymerase proofreading-associated polyposis (PPAP).
We screened for mutations in patients with multiple adenomas/FAP: 121 patients were analyzed for APC and MUTYH mutations, and 36 patients were also evaluated for POLE and POLD1 gene mutations.
We found 20 FAP/AFAP, 15 MAP, and no PPAP subjects: pathogenic mutations proved to be heterogeneous, and included 5 APC and 1 MUTYH novel mutations. The mutation detection rate was significantly different between patients with 5-100 polyps and those with >100 polyps (p = 8.154 × 10), with APC mutations being associated with an aggressive phenotype (p = 1.279 × 10). Mean age at diagnosis was lower in FAP/AFAP compared to MAP (p = 3.055 × 10). Mutation-negative probands showed a mean age at diagnosis that was significantly higher than FAP/AFAP (p = 3.46986 × 10) and included 45.3% of patients with <30 polyps and 70.9% of patients with no family history.
This study enlarges the APC and MUTYH mutational spectra, and also evaluated variants of uncertain significance, including the MUTYH p.Gln338His mutation. Moreover this study underscores the phenotypic heterogeneity and genotype-phenotype correlations in a cohort of Italian patients.
导致癌症易感性的结直肠腺瘤性息肉病由不同基因的胚系突变引起。APC与家族性腺瘤性息肉病(FAP/AFAP)相关,MUTYH与MUTYH相关息肉病(MAP)相关,而POLE和POLD1突变导致聚合酶校对相关息肉病(PPAP)。
我们对患有多个腺瘤/FAP的患者进行了突变筛查:对121例患者分析了APC和MUTYH突变,对36例患者还评估了POLE和POLD1基因突变。
我们发现了20例FAP/AFAP、15例MAP患者,未发现PPAP患者:致病性突变证明是异质性的,包括5个APC和1个MUTYH新突变。息肉数为5 - 100个的患者与息肉数>100个的患者之间的突变检出率有显著差异(p = 8.154×10),APC突变与侵袭性表型相关(p = 1.279×10)。FAP/AFAP患者的诊断平均年龄低于MAP患者(p = 3.055×10)。突变阴性的先证者诊断时的平均年龄显著高于FAP/AFAP患者(p = 3.46986×10),其中息肉数<30个的患者占45.3%,无家族史的患者占70.9%。
本研究扩大了APC和MUTYH的突变谱,还评估了意义未明的变异,包括MUTYH p.Gln338His突变。此外,本研究强调了一组意大利患者中的表型异质性和基因型 - 表型相关性。
