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Fusion, gene misexpression and homeotic transformations in vertebral development of the gnathostome stem group (Placodermi)

机译:gnathostome茎组(Placodermi)椎骨发育中的融合,基因错误表达和同源转换

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Development of the vertebral column is controlled by a complex of pleiotropic and polygenetic phenomena, in the mouse and chick regulating formation of different parts of individual vertebrae and morphological identity along the column (‘Hox code’). In mouse and chick, experimental misexpression, including upstream and downstream genes, results in shifts in vertebral identity, loss of particular parts of individual vertebrae or vertebral fusion. Axial skeleton homologies across the Vertebrata allow these observations to be extended to taxa such as Homo sapiens, Chondrichthyes and Placodermi, the latter an entirely fossil group. Misexpression phenotypes among fossil taxa illuminate the phylogenetic history of these regulatory mechanisms. Phenotypes associated with genes originating via genomic duplication can determine the historical depth for these duplication events. Analysis of an ontogenetic sequence for the occipital-synarcual complex in the placoderm Cowralepis mclachlani provides the basis for comparison of this early gnathostome with other placoderms, chondrichthyans and amniotes. The occipital-synarcual patterns in placoderms parallel the phenotypic misexpression in mice and chicks (fusion and homeotic mutation) and the varying degrees of fusion in the Type I-III human Klippel-Feil syndrome. The association of these phenotypes to Hoxd regulatory complexes indicates that the gnathostome genomic duplication occurred at the base of the gnathostome stem group. Given the conservative nature of regulatory genes and the homology of vertebral elements, the presence of fusion in stem gnathostomes implies that the mechanism of fusion in mouse and chick models can be extrapolated to extant chondrichthyans (testable) and accounts for the phenotypic similarity across gnathostomes. The presence of these phenotypes in fossils indicates the antiquity of these regulatory mechanisms and of genomic duplication.
机译:脊柱的发育受多效性和多基因现象的综合影响,在小鼠和雏鸡中,调节单个椎骨不同部分的形成和沿该柱的形态特征(“ Hox码”)。在小鼠和雏鸡中,包括上游和下游基因在内的实验性错误表达会导致椎骨同一性的改变,单个椎骨特定部位的丢失或椎骨融合。整个椎骨上的轴向骨骼同源性使得这些观测结果可以扩展到生物群,例如智人,软骨鱼类和Placodermi,后者完全是化石群。化石类群中的错误表达表型阐明了这些调节机制的系统发育史。与通过基因组复制起源的基因相关的表型可以确定这些复制事件的历史深度。对齿coder母牛Cowralepis mclachlani中枕-鼻交复合体的个体发育序列的分析,为该早期的gnathostome与其他齿,软骨鱼类和羊膜的比较提供了基础。编轴器中枕骨-性交的模式与小鼠和雏鸡的表型错误表达(融合和同源突变)以及I-III型人Klippel-Feil综合征的融合程度不同。这些表型与Hoxd调节复合体的关联表明,gnathostome基因组重复发生在gnathostome干群的底部。鉴于调节基因的保守性质和椎骨元素的同源性,在茎生器动物中融合的存在意味着可以将小鼠和雏鸡模型中的融合机制外推至现存的软骨鱼类(可测试),并解释了整个生器动物的表型相似性。化石中这些表型的存在表明了这些调节机制和基因组重复的古代。

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