using paleogenomics to study the evolution of gene families origin and duplication history of the relaxin family hormones and their receptors使用paleogenomics研究基因家族的进化起源和重复历史松弛素家族的激素及其受体.pdfVIP

using paleogenomics to study the evolution of gene families origin and duplication history of the relaxin family hormones and their receptors使用paleogenomics研究基因家族的进化起源和重复历史松弛素家族的激素及其受体.pdf

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using paleogenomics to study the evolution of gene families origin and duplication history of the relaxin family hormones and their receptors使用paleogenomics研究基因家族的进化起源和重复历史松弛素家族的激素及其受体

Using Paleogenomics to Study the Evolution of Gene Families: Origin and Duplication History of the Relaxin Family Hormones and Their Receptors Sergey Yegorov, Sara Good* Department of Biology, University of Winnipeg, Winnipeg, Manitoba, Canada Abstract Recent progress in the analysis of whole genome sequencing data has resulted in the emergence of paleogenomics, a field devoted to the reconstruction of ancestral genomes. Ancestral karyotype reconstructions have been used primarily to illustrate the dynamic nature of genome evolution. In this paper, we demonstrate how they can also be used to study individual gene families by examining the evolutionary history of relaxin hormones (RLN/INSL) and relaxin family peptide receptors (RXFP). Relaxin family hormones are members of the insulin superfamily, and are implicated in the regulation of a variety of primarily reproductive and neuroendocrine processes. Their receptors are G-protein coupled receptors (GPCR’s) and include members of two distinct evolutionary groups, an unusual characteristic. Although several studies have tried to elucidate the origins of the relaxin peptide family, the evolutionary origin of their receptors and the mechanisms driving the diversification of the RLN/INSL-RXFP signaling systems in non-placental vertebrates has remained elusive. Here we show that the numerous vertebrate RLN/INSL and RXFP genes are products of an ancestral receptor-ligand system that originally consisted of three genes, two of which apparently trace their origins to invertebrates. Subsequently, diversification of the system was driven primarily by whole genome duplications (WGD, 2R and 3R) followed by almost complete retention of the ligand duplicates in most vertebrates but massive loss of receptor genes in tetrapods. Interestingly, the majority of 3R duplicates retained in

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