戈林综合征中刺猬相关基因的多层突变可能影响表型。
Multi-layered mutation in hedgehog-related genes in Gorlin syndrome may affect the phenotype.
作者信息
Onodera Shoko, Saito Akiko, Hasegawa Daigo, Morita Nana, Watanabe Katsuhito, Nomura Takeshi, Shibahara Takahiko, Ohba Shinsuke, Yamaguchi Akira, Azuma Toshifumi
机构信息
Department of Biochemistry, Tokyo Dental College, Tokyo, Japan.
Division of Clinical Biotechnology, The University of Tokyo Graduate School of Medicine, Bunkyo-ku, Tokyo, Japan; Department of Bioengineering, The University of Tokyo Graduate School of Engineering, Bunkyo-ku, Tokyo, Japan.
出版信息
PLoS One. 2017 Sep 15;12(9):e0184702. doi: 10.1371/journal.pone.0184702. eCollection 2017.
Gorlin syndrome is a genetic disorder of autosomal dominant inheritance that predisposes the affected individual to a variety of disorders that are attributed largely to heterozygous germline patched1 (PTCH1) mutations. PTCH1 is a hedgehog (Hh) receptor as well as a repressor, mutation of which leads to constitutive activation of Hh pathway. Hh pathway encompasses a wide variety of cellular signaling cascades, which involve several molecules; however, no associated genotype-phenotype correlations have been reported. Recently, mutations in Suppressor of fused homolog (SUFU) or PTCH2 were reported in patients with Gorlin syndrome. These facts suggest that multi-layered mutations in Hh pathway may contribute to the development of Gorlin syndrome. We demonstrated multiple mutations of Hh-related genes in addition to PTCH1, which possibly act in an additive or multiplicative manner and lead to Gorlin syndrome. High-throughput sequencing was performed to analyze exome sequences in four unrelated Gorlin syndrome patient genomes. Mutations in PTCH1 gene were detected in all four patients. Specific nucleotide variations or frameshift variations of PTCH1 were identified along with the inferred amino acid changes in all patients. We further filtered 84 different genes which are closely related to Hh signaling. Fifty three of these had enough coverage of over ×30. The sequencing results were filtered and compared to reduce the number of sequence variants identified in each of the affected individuals. We discovered three genes, PTCH2, BOC, and WNT9b, with mutations with a predicted functional impact assessed by MutationTaster2 or PolyPhen-2 (Polymorphism Phenotyping v2) analysis. It is noticeable that PTCH2 and BOC are Hh receptor molecules. No significant mutations were observed in SUFU. Multi-layered mutations in Hh pathway may change the activation level of the Hh signals, which may explain the wide phenotypic variability of Gorlin syndrome.
戈林综合征是一种常染色体显性遗传的基因紊乱疾病,使受影响个体易患多种疾病,这些疾病主要归因于杂合性种系patched1(PTCH1)突变。PTCH1是一种刺猬信号通路(Hh)受体,也是一种阻遏物,其突变会导致Hh信号通路的组成性激活。Hh信号通路包含多种细胞信号级联反应,涉及多个分子;然而,尚未有相关基因型-表型相关性的报道。最近,在戈林综合征患者中报道了融合抑制同源物(SUFU)或PTCH2的突变。这些事实表明,Hh信号通路中的多层突变可能导致戈林综合征的发生。我们证明了除PTCH1外,Hh相关基因的多个突变,这些突变可能以累加或倍增的方式起作用,导致戈林综合征。对4名无关的戈林综合征患者基因组进行高通量测序以分析外显子序列。在所有4名患者中均检测到PTCH1基因突变。在所有患者中均鉴定出PTCH1的特定核苷酸变异或移码变异以及推断的氨基酸变化。我们进一步筛选了84个与Hh信号密切相关的不同基因。其中53个基因的覆盖度足够高,超过了30倍。对测序结果进行筛选和比较,以减少每个受影响个体中鉴定出的序列变异数量。我们发现了3个基因,即PTCH2、BOC和WNT9b,通过MutationTaster2或PolyPhen-2(多态性表型分析v2)分析评估,这些基因的突变具有预测的功能影响。值得注意的是,PTCH2和BOC是Hh受体分子。在SUFU中未观察到显著突变。Hh信号通路中的多层突变可能会改变Hh信号的激活水平,这可能解释了戈林综合征广泛的表型变异性。
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