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长臂猿基因组重排的分子精细化

Molecular refinement of gibbon genome rearrangements.

作者信息

Roberto Roberta, Capozzi Oronzo, Wilson Richard K, Mardis Elaine R, Lomiento Mariana, Tuzun Eray, Cheng Ze, Mootnick Alan R, Archidiacono Nicoletta, Rocchi Mariano, Eichler Evan E

机构信息

Department of Genetics and Microbiology, University of Bari, 70126 Bari, Italy.

出版信息

Genome Res. 2007 Feb;17(2):249-57. doi: 10.1101/gr.6052507. Epub 2006 Dec 21.

Abstract

The gibbon karyotype is known to be extensively rearranged when compared to the human and to the ancestral primate karyotype. By combining a bioinformatics (paired-end sequence analysis) approach and a molecular cytogenetics approach, we have refined the synteny block arrangement of the white-cheeked gibbon (Nomascus leucogenys, NLE) with respect to the human genome. We provide the first detailed clone framework map of the gibbon genome and refine the location of 86 evolutionary breakpoints to <1 Mb resolution. An additional 12 breakpoints, mapping primarily to centromeric and telomeric regions, were mapped to approximately 5 Mb resolution. Our combined FISH and BES analysis indicates that we have effectively subcloned 49 of these breakpoints within NLE gibbon BAC clones, mapped to a median resolution of 79.7 kb. Interestingly, many of the intervals associated with translocations were gene-rich, including some genes associated with normal skeletal development. Comparisons of NLE breakpoints with those of other gibbon species reveal variability in the position, suggesting that chromosomal rearrangement has been a longstanding property of this particular ape lineage. Our data emphasize the synergistic effect of combining computational genomics and cytogenetics and provide a framework for ultimate sequence and assembly of the gibbon genome.

摘要

与人类和灵长类祖先核型相比,长臂猿核型发生了广泛重排。通过结合生物信息学(双末端序列分析)方法和分子细胞遗传学方法,我们完善了白颊长臂猿(Nomascus leucogenys, NLE)与人类基因组的同线性区段排列。我们提供了首个详细的长臂猿基因组克隆框架图,并将86个进化断点的定位精度提高到小于1 Mb,另外12个主要定位于着丝粒和端粒区域的断点定位精度约为5 Mb。我们结合荧光原位杂交(FISH)和细菌人工染色体末端测序(BES)分析表明,我们已在NLE长臂猿BAC克隆中有效亚克隆了其中49个断点,定位的中位分辨率为79.7 kb。有趣的是,许多与易位相关的区间富含基因,包括一些与正常骨骼发育相关的基因。将NLE断点与其他长臂猿物种的断点进行比较,发现位置存在差异,这表明染色体重排是这一特定猿类谱系的长期特征。我们的数据强调了结合计算基因组学和细胞遗传学的协同效应,并为长臂猿基因组的最终测序和组装提供了框架。

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