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内皮素系统:通过三轮基因组复制实现脊椎动物特异性配体 - 受体相互作用的进化。

The endothelin system: evolution of vertebrate-specific ligand-receptor interactions by three rounds of genome duplication.

作者信息

Braasch Ingo, Volff Jean-Nicolas, Schartl Manfred

机构信息

University of Würzburg, Biozentrum, Physiological Chemistry I, Germany.

出版信息

Mol Biol Evol. 2009 Apr;26(4):783-99. doi: 10.1093/molbev/msp015. Epub 2009 Jan 27.

Abstract

Morphological innovations like the acquisition of the neural crest as well as gene family expansions by genome duplication are considered as major leaps in the evolution of the vertebrate lineage. Using comparative genomic analyses, we have reconstructed the evolutionary history of the endothelin system, a signaling pathway consisting of endothelin ligands and their G protein-coupled receptors. The endothelin system plays a key role in cardiovascular regulation as well as in the development of diverse neural crest derivatives like pigment cells and craniofacial bone structures, which are hot spots of diversity in vertebrates. However, little is known about the origin and evolution of the endothelin system in the vertebrate lineage. We show that the endothelin core system, that is, endothelin ligands (Edn) and their receptors (Ednr), is a vertebrate-specific innovation. The components of the endothelin core system in modern vertebrate genomes date back to single genes that have been duplicated during whole-genome duplication events. After two rounds of genome duplication during early vertebrate evolution, the endothelin system of an ancestral gnathostome consisted of four ligand and four receptor genes. The previously unknown fourth endothelin ligand Edn4 has been kept in teleost fish but lost in tetrapods. Bony vertebrates generally possess three receptor genes, EdnrA, EdnrB1, and EdnrB2. EdnrB2 has been lost secondarily in the mammalian lineage from a chromosome that gave rise to the sex chromosomes in therians (marsupials and placentals). The endothelin system of fishes was further expanded by a fish-specific genome duplication and duplicated edn2, edn3, ednrA, and ednrB1 genes have been retained in teleost fishes. Functional divergence analyses suppose that following each round of genome duplication, coevolution of ligands and their binding regions in the receptors has occurred, adjusting the endothelin signaling system to the increase of possible ligand-receptor interactions. Furthermore, duplications of genes involved in the endothelin system are associated with functional specialization for the development of particular neural crest derivatives. Our results support an important role for newly emerging ligands and receptors as components of signaling pathways and their expansion through genome duplications in the evolution of the vertebrate neural crest.

摘要

形态学创新,如神经嵴的获得以及通过基因组复制实现的基因家族扩张,被认为是脊椎动物谱系进化中的重大飞跃。通过比较基因组分析,我们重建了内皮素系统的进化史,内皮素系统是一种由内皮素配体及其G蛋白偶联受体组成的信号通路。内皮素系统在心血管调节以及多种神经嵴衍生物(如色素细胞和颅面骨结构)的发育中起关键作用,而这些衍生物是脊椎动物多样性的热点。然而,关于脊椎动物谱系中内皮素系统的起源和进化,我们所知甚少。我们发现,内皮素核心系统,即内皮素配体(Edn)及其受体(Ednr),是脊椎动物特有的创新。现代脊椎动物基因组中内皮素核心系统的组成部分可追溯到在全基因组复制事件中发生复制的单个基因。在早期脊椎动物进化过程中经历两轮基因组复制后,一个原始有颌类动物的内皮素系统由四个配体基因和四个受体基因组成。此前未知的第四个内皮素配体Edn4在硬骨鱼中得以保留,但在四足动物中丢失。硬骨脊椎动物通常拥有三个受体基因,即EdnrA、EdnrB1和EdnrB2。EdnrB2在哺乳动物谱系中从一条产生有袋类动物和胎盘类动物性染色体的染色体上再次丢失。鱼类的内皮素系统通过一次鱼类特有的基因组复制进一步扩展,复制后的edn2、edn3、ednrA和ednrB1基因在硬骨鱼中得以保留。功能差异分析表明,在每一轮基因组复制之后,配体及其在受体中的结合区域发生了共同进化,使内皮素信号系统适应可能的配体 - 受体相互作用的增加。此外,内皮素系统中相关基因的复制与特定神经嵴衍生物发育的功能特化有关。我们的研究结果支持了新出现的配体和受体作为信号通路组成部分及其通过基因组复制在脊椎动物神经嵴进化中的扩张所起的重要作用。

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