在一个有家族性腺瘤性息肉病的泰国南部家庭中发现了一种独特的 APC 致病性种系变异。
A distinct APC pathogenic germline variant identified in a southern Thai family with familial adenomatous polyposis.
机构信息
Department of Surgery, Faculty of Medicine, Prince of Songkla University, Songkhla, 90110, Thailand.
Department of Ophthalmology, Faculty of Medicine, Prince of Songkla University, Songkhla, 90110, Thailand.
出版信息
BMC Med Genomics. 2021 Mar 19;14(1):87. doi: 10.1186/s12920-021-00933-y.
BACKGROUND
Familial adenomatous polyposis (FAP) is caused by pathogenic germline variants in the APC gene. To date, multiple pathogenic variants in coding regions, splice sites, and deep intronic regions have been revealed. However, there are still pathogenic variants that remain unidentified.
METHODS
Twenty-nine primer pairs flanking exons 2-16 (i.e., coding exons 1-15) of APC and their exon-intron junctions were used for germline pathogenic variant screening in Southern Thai patients with familial adenomatous polyposis (FAP). Transcription analysis was performed to confirm the pathogenicity of a splice site deletion of intron 10. Family members were interviewed for clinical histories. Blood samples were collected from 18 family members for a segregation study. Subsequently, clinical data of affected members were collected from the hospital databases.
RESULTS
We found a distinct heterozygous 16-bp deletion at the splice donor site of intron 10 leading to a skipping of exon 10 which was confirmed by transcript analysis (APC: c 1312 + 4_1312 + 19del, r.934_1312del). Predictive testing for the pathogenic APC variant in 18 of the proband's family members (ten healthy and eight affected) from three generations showed the same heterozygous germline pathogenic variant in eight affected adult members (15-62 years old) and two children (7 and 10 years old). Seven of the ten carriers of the disease-causing variant had undergone colonoscopy, and colonic polyps were found in all cases, which confirmed the segregation of the inherited pathogenic variant. The phenotypic spectrum was found to vary within the family; and some affected family members exhibited extracolonic manifestations.
CONCLUSIONS
To our knowledge, the pathogenic APC variant, c.1312 + 4_1312 + 19del, r.934_1312del, has not previously been reported. This study is one of the few reports describing the phenotypic consequences of a pathogenic APC variant in a high number of affected family members.
背景
家族性腺瘤性息肉病(FAP)是由 APC 基因的致病性种系变异引起的。迄今为止,已经发现了编码区域、剪接位点和深内含子区域的多种致病性变异,但仍有一些致病性变异尚未确定。
方法
使用 29 对侧翼 APC 外显子 2-16(即编码外显子 1-15)及其外显子-内含子交界处的引物对,对来自泰国南部的家族性腺瘤性息肉病(FAP)患者进行种系致病性变异筛查。进行转录分析以确认 10 号内含子剪接供体位点缺失的致病性。对家族成员进行临床病史访谈。从 18 个家族成员采集血液样本进行分离研究。随后,从医院数据库中收集受影响成员的临床数据。
结果
我们发现了一个明显的杂合 16 个碱基对缺失,位于 10 号内含子的剪接受体位点,导致外显子 10 跳跃,这通过转录分析得到证实(APC:c.1312+4_1312+19del,r.934_1312del)。对先证者的 18 个家族成员(10 个健康和 8 个受影响)进行了 APC 致病性变异的预测性检测,结果显示,在 8 个成年受影响成员(15-62 岁)和 2 个儿童(7 和 10 岁)中存在相同的杂合种系致病性变异。携带致病变异的 10 个携带者中有 7 人接受了结肠镜检查,所有病例均发现结肠息肉,证实了遗传致病性变异的分离。发现家族内的表型谱存在差异;一些受影响的家族成员还存在结肠外表现。
结论
据我们所知,该致病性 APC 变异 c.1312+4_1312+19del,r.934_1312del,以前没有报道过。本研究是为数不多的描述大量受影响家族成员中 APC 致病性变异的表型后果的研究之一。
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