Division of Nephrology and Hypertension, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA.
Hum Genet. 2011 Mar;129(3):345-9. doi: 10.1007/s00439-011-0950-8. Epub 2011 Jan 28.
The autosomal recessive polycystic kidney disease (ARPKD) gene, PKHD1, has been implicated in the genesis or growth of colorectal adenocarcinoma, as a high level of somatic mutations was found in colorectal tumor tissue. To determine whether carriers of a single PKHD1 mutation are at increased risk of colorectal carcinoma, we assessed the prevalence of the commonest European mutation, T36M. First, we assayed a European cohort of ARPKD patients and found T36M was responsible for 13.1% of mutations. We then investigated two European cohorts with colorectal adenocarcinoma versus two control cohorts of similar age and gender. Screening for the most common PKHD1 mutation, T36M, we detected 15:3,603 (0.42%) controls versus 1:3,767 (0.027%) colorectal cancer individuals, indicating that heterozygous PKHD1 mutations are not a risk factor and are protective (p=0.0002). We also show that the carriage rate for PKHD1 mutations in the European population is higher than previous accepted at 3.2% (1:31 genomes).
常染色体隐性多囊肾病 (ARPKD) 基因 PKHD1 与结直肠腺癌的发生或生长有关,因为在结直肠肿瘤组织中发现了高水平的体细胞突变。为了确定携带单个 PKHD1 突变的个体是否有更高的结直肠癌风险,我们评估了最常见的欧洲突变 T36M 的流行率。首先,我们检测了一个欧洲 ARPKD 患者队列,发现 T36M 导致 13.1%的突变。然后,我们调查了两个具有结直肠腺癌的欧洲队列和两个具有相似年龄和性别的对照队列。筛查最常见的 PKHD1 突变 T36M,我们在 15:3,603 名对照者(0.42%)中检测到,在 3,767 名结直肠癌个体(0.027%)中检测到,表明杂合性 PKHD1 突变不是风险因素而是保护因素(p=0.0002)。我们还表明,PKHD1 突变在欧洲人群中的携带率高于先前接受的 3.2%(1:31 个基因组)。