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硬骨鱼中重复的hoxb5基因的功能解析

Functional resolution of duplicated hoxb5 genes in teleosts.

作者信息

Jarinova Olga, Hatch Gary, Poitras Luc, Prudhomme Christelle, Grzyb Magdalena, Aubin Josée, Bérubé-Simard Félix-Antoine, Jeannotte Lucie, Ekker Marc

机构信息

Center for Advanced Research in Environmental Genomics, Department of Biology, University of Ottawa, Ottawa, Ontario K1N 6N5, Canada.

出版信息

Development. 2008 Nov;135(21):3543-53. doi: 10.1242/dev.025817. Epub 2008 Oct 2.

DOI:10.1242/dev.025817
PMID:18832391
Abstract

The duplication-degeneration-complementation (DDC) model predicts that subfunctionalization of duplicated genes is a common mechanism for their preservation. The additional Hox complexes of teleost fish constitute a good system in which to test this hypothesis. Zebrafish have two hoxb complexes, with two hoxb5 genes, hoxb5a and hoxb5b, the expression patterns of which suggest subfunctionalization of an ancestral hoxb5 gene. We characterized conserved non-coding elements (CNEs) near the zebrafish hoxb5 genes. One CNE, J3, is only retained in the hoxb5a locus, whereas the others, J1 and J2, are present in both hoxb5 loci. When tested individually, the enhancer activity of individual CNEs, including J3, extensively overlapped and did not support a role in subfunctionalization. By contrast, reporter transgene constructs encompassing multiple CNEs were able to target reporter gene expression to unique domains of hoxb5a and hoxb5b expression. The deletion of J3 from the hoxb5a locus resulted in expression that approached that of hoxb5b, whereas its insertion in the hoxb5b locus increased reporter expression and rendered it more similar to that of hoxb5a. Our results highlight the importance of interactions between CNEs in the execution of complementary subfunctions of duplicated genes.

摘要

重复-退化-互补(DDC)模型预测,重复基因的亚功能化是其得以保留的常见机制。硬骨鱼额外的Hox复合体构成了一个验证这一假说的良好系统。斑马鱼有两个hoxb复合体,其中有两个hoxb5基因,即hoxb5a和hoxb5b,它们的表达模式表明一个祖先hoxb5基因发生了亚功能化。我们对斑马鱼hoxb5基因附近的保守非编码元件(CNE)进行了特征分析。一个CNE,即J3,仅保留在hoxb5a基因座中,而其他的J1和J2在两个hoxb5基因座中均存在。单独测试时,包括J3在内的各个CNE的增强子活性广泛重叠,并不支持其在亚功能化中起作用。相比之下,包含多个CNE的报告转基因构建体能够将报告基因的表达靶向到hoxb5a和hoxb5b表达的独特结构域。从hoxb5a基因座中删除J3导致其表达接近hoxb5b的表达,而将其插入hoxb5b基因座则增加了报告基因的表达,并使其更类似于hoxb5a的表达。我们的结果突出了CNE之间的相互作用在重复基因互补亚功能执行中的重要性。

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