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CCND1 polymorphism and age of onset of hepatoblastoma

机译:CCND1基因多态性与肝母细胞瘤的发病年龄

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摘要

Cyclin D1, encoded by the gene CCND1, is a major regulator of the cell cycle transition from G1 phase to S phase. A CCND1 polymorphism (G to A) at codon 242, the boundary of exon 4 and intron 4, affects splicing such that exon 5 is not expressed in the A allele. Since exon 5 is involved in rapid turnover, the variant cyclin D1 corresponding to the A allele may have a longer half-life. A previous study demonstrated that in families with hereditary nonpolyposis colorectal cancer, the age of onset of colorectal cancer varied according to variation at this polymorphic site. We examined this CCND1polymorphism in a series hepatoblastoma, a childhood liver cancer that shares other molecular features with colon cancer. We determined in an analysis of 84 children with hepatoblastoma that the G/A exon 4 polymorphism in CCND1 is correlated with the age of onset of hepatoblastomas. The A/A genotype is associated with an earlier age of onset compared to the G/A or G/G genotype. The median age of patients with the G/G genotype was 22 months, compared to 17 months in patients with the G/A genotype and 11 months for the A/A genotype. These findings suggest that the CCND1 A polymorphism may contribute to tumor development in children with hepatoblastoma.
机译:由基因CCND1编码的细胞周期蛋白D1是细胞周期从G1期过渡到S期的主要调节剂。密码子242(外显子4和内含子4的边界)处的CCND1多态性(G到A)影响剪接,因此外显子5在A等位基因中不表达。由于外显子5参与快速周转,因此对应于A等位基因的变体细胞周期蛋白D1可能具有更长的半衰期。先前的研究表明,在患有遗传性非息肉病大肠癌的家庭中,大肠癌的发病年龄根据该多态性位点的变异而有所不同。我们在一系列肝母细胞瘤(一种儿童期肝癌,与结肠癌具有其他分子特征)中研究了CCND1多态性。我们在对84例肝母细胞瘤儿童的分析中确定,CCND1中的G / A外显子4多态性与肝母细胞瘤的发病年龄相关。与G / A或G / G基因型相比,A / A基因型与发病年龄早。 G / G基因型患者的中位年龄为22个月,而G / A基因型患者为17个月,A / A基因型患者为11个月。这些发现表明,CCND1 A基因多态性可能有助于肝母细胞瘤儿童的肿瘤发展。

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