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Estimate of de novo mutation frequency in probands with PTEN hamartoma tumor syndrome

机译:PTEN错构瘤肿瘤综合征先证者从头突变频率的估计

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Purpose:PTEN hamartoma tumor syndrome is an autosomal dominant disorder with increased risks of neoplasias, macrocephaly, and developmental disabilities. While both familial and sporadic cases exist, actual de novo mutation frequency remains unknown. We sought to estimate this within our PTEN-mutation positive patient series.Methods:Patients were prospectively accrued if they had known pathogenic germline PTEN mutations or phenotypic features suspicious for PHTS. Only families with pathogenic PTEN mutations were included. Likelihood for de novo mutation was graded from 1 (confirmed inherited) to 5 (confirmed de novo) based on family history and mutation status. Fishers two-tailed exact and unpaired t-tests were used to compare between groups.Results:187 pathogenic PTEN-mutation positive families were eligible for this study. De novo (grade 5) status was confirmed in 20 (10.7%) probands, and in 36 (19.3%) was suspected based on family history. Demographics, mutations, and phenotypes were similar for probands graded 1 vs. 5 (all P>0.06). In grade 1 probands, mutations were inherited equally from maternal and paternal lineages (P = 0.55).Conclusions:The frequency of de novo PTEN mutation is at minimum 10.7% and at best 47.6%. Absence of PHTS features within a family history should not preclude consideration of this diagnosis for patients with relevant personal history.
机译:目的:PTEN错构瘤肿瘤综合征是一种常染色体显性遗传疾病,伴有瘤形成,大头畸形和发育障碍的风险增加。虽然家族和散发病例都存在,但实际的从头突变频率仍然未知。我们试图在我们的PTEN突变阳性患者系列中对此进行估计。仅包括具有致病性PTEN突变的家庭。根据家族史和突变状态,从头突变的可能性从1(确认继承)到5(从头确认)分级。结果:187个致病性PTEN突变阳性家庭符合本研究的要求。从20个(10.7%)先证者中确认为从头(5年级)状态,根据家族史,怀疑有36个(19.3%)的先证者。 1级对5级先证者的人口统计学,突变和表型相似(所有P> 0.06)。在1级先证者中,突变从母系和父系中均等地遗传(P = 0.55)。结论:从头PTEN突变的频率最低为10.7%,最高为47.6%。家族史中没有PHTS功能的患者,不应排除对具有相关个人史的患者进行此诊断的考虑。

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