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人类染色体11q和21q复制时间的全染色体评估:时间转换区域中的疾病相关基因

Chromosome-wide assessment of replication timing for human chromosomes 11q and 21q: disease-related genes in timing-switch regions.

作者信息

Watanabe Yoshihisa, Fujiyama Asao, Ichiba Yuta, Hattori Masahira, Yada Tetsushi, Sakaki Yoshiyuki, Ikemura Toshimichi

机构信息

Division of Evolutionary Genetics, Department of Population Genetics, National Institute of Genetics, Yata 1111, Mishima, Shizuoka-ken 411-8540, Japan.

出版信息

Hum Mol Genet. 2002 Jan 1;11(1):13-21. doi: 10.1093/hmg/11.1.13.

DOI:10.1093/hmg/11.1.13
PMID:11772995
Abstract

The completion of the human genome sequence will greatly accelerate development of a new branch of bioscience and provide fundamental knowledge to biomedical research. We used the sequence information to measure replication timing of the entire lengths of human chromosomes 11q and 21q. Megabase-sized zones that replicate early or late in S phase (thus early/late transition) were defined at the sequence level. Early zones were more GC-rich and gene-rich than were late zones, and early/late transitions occurred primarily at positions identical to or near GC% transitions. We also found the single nucleotide polymorphism (SNP) frequency was high in the late-replicating and replication-transition regions. In the early/late transition regions, concentrated occurrence of cancer-related genes that include CCND1 encoding cyclin D1 (BCL1), FGF4 (KFGF), TIAM1 and FLI1, was observed. The transition regions contained other disease-related genes including APP associated with familial Alzheimer's disease (AD1), SOD1 associated with familial amyotrophic lateral sclerosis (ALS1) and PTS associated with phenylketonuria. These findings are discussed with respect to the prediction that increased DNA damage occurs in replication-transition regions. We propose that genome-wide assessment of replication timing serves as an efficient strategy for identifying disease-related genes.

摘要

人类基因组序列的完成将极大地加速生物科学一个新分支的发展,并为生物医学研究提供基础知识。我们利用该序列信息来测量人类11号染色体长臂和21号染色体长臂全长的复制时间。在序列水平上定义了在S期早期或晚期复制的兆碱基大小区域(即早期/晚期转换)。早期区域比晚期区域富含更多的GC且基因更丰富,早期/晚期转换主要发生在与GC%转换相同或接近的位置。我们还发现单核苷酸多态性(SNP)频率在晚期复制和复制转换区域较高。在早期/晚期转换区域,观察到包括编码细胞周期蛋白D1(BCL1)的CCND1、FGF4(KFGF)、TIAM1和FLI1等癌症相关基因的集中出现。转换区域还包含其他疾病相关基因,包括与家族性阿尔茨海默病(AD1)相关的APP、与家族性肌萎缩侧索硬化症(ALS1)相关的SOD1以及与苯丙酮尿症相关的PTS。针对复制转换区域发生DNA损伤增加这一预测对这些发现进行了讨论。我们提出全基因组复制时间评估是识别疾病相关基因的有效策略。

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