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首页> 外文期刊>European journal of human genetics: EJHG >Linkage analysis revealed risk loci on 6p21 and 18p11.2-q11.2 in familial colon and rectal cancer, respectively
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Linkage analysis revealed risk loci on 6p21 and 18p11.2-q11.2 in familial colon and rectal cancer, respectively

机译:联动分析显示在家族性结肠和直肠癌中的6P21和18P11.2-Q11.2上显示出风险基因座

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Colorectal cancer (CRC) is one of the major cancer types in the western world including Sweden. However, known genetic risk factors could only explain a limited part of heritability of the disease. Moreover, colon and rectal cancers are habitually discussed as one entity, colorectal cancer, although different carcinogenesis has been recognized. A genome-wide linkage scan in 32 colon- and 56 rectal cancer families from Sweden was performed based on 475 non-FAP/HNPCC patients genotyped using SNP arrays. A maximum HLOD of 2.50 at locus 6p21.1-p12.1 and a HLOD of 2.56 at 18p11.2 was obtained for colon and rectal cancer families, respectively. Exome sequencing over the regions of interest in 12 patients from six families identified 22 and 25 candidate risk variants for colon and rectal cancer, respectively. Haplotype association analysis in the two regions was carried out between additional 477 familial CRC cases and 4780 controls and suggested candidate haplotypes possibly associated with CRC risk. This study suggested two new linkage regions for colon cancer and rectal cancer with candidate predisposing variants. Further studies are required to elucidate the pathogenic mechanism of these regions and to pinpoint the causative genes.
机译:结肠直肠癌(CRC)是西方世界的主要癌症类型之一,包括瑞典。然而,已知的遗传危险因素只能解释疾病的有限部分。此外,结肠和直肠癌习惯性地讨论为一个实体,结直肠癌,尽管已经认识到不同的致癌作用。基于使用SNP阵列的475个非FAP / HNPCC患者进行32种来自瑞典的结肠和56个直肠癌族的基因组连接扫描。对于结肠和直肠癌家族,获得了110P21.1-P12.1的最大HLOD 2.50.18P11.2的HLOD。在六个家庭的12名患者中,exome测序分别鉴定了22例患者的结肠癌和直肠癌25名候选风险变体。两种区域的单倍型关联分析在另外的477个家族性CRC病例和4780个对照之间进行,并建议候选单倍型可能与CRC风险相关。该研究表明,具有候选概念性的结肠癌和直肠癌的两种新的联系区域。需要进一步的研究来阐明这些区域的致病机制并确定致病基因。

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