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Expansion of Secretin-Like G Protein-Coupled Receptors and Their Peptide Ligands via Local Duplications Before and After Two Rounds of Whole-Genome Duplication

Authors
Hwang, Jong-IkMoon, Mi JinPark, SumiKim, Dong-KyuCho, Eun BeeHa, NuiSon, Gi HoonKim, KyungjinVaudry, HubertSeong, Jae Young
Issue Date
5월-2013
Publisher
OXFORD UNIV PRESS
Keywords
secretin; G protein-coupled receptor; genome; comparative genomics; evolution; genome duplication
Citation
MOLECULAR BIOLOGY AND EVOLUTION, v.30, no.5, pp.1119 - 1130
Indexed
SCIE
SCOPUS
Journal Title
MOLECULAR BIOLOGY AND EVOLUTION
Volume
30
Number
5
Start Page
1119
End Page
1130
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/103335
DOI
10.1093/molbev/mst031
ISSN
0737-4038
Abstract
In humans, the secretin-like G protein-coupled receptor (GPCR) family comprises 15 members with 18 corresponding peptide ligand genes. Although members have been identified in a large variety of vertebrate and nonvertebrate species, the origin and relationship of these proteins remain unresolved. To address this issue, we employed large-scale genome comparisons to identify genome fragments with conserved synteny and matched these fragments to linkage groups in reconstructed early gnathostome ancestral chromosomes (GAC). This genome comparison revealed that most receptor and peptide genes were clustered in three GAC linkage groups and suggested that the ancestral forms of five peptide subfamilies (corticotropin-releasing hormone-like, calcitonin-like, parathyroid hormone-like, glucagon-like, and growth hormone-releasing hormone-like) and their cognate receptor families emerged through tandem local gene duplications before two rounds (2R) of whole-genome duplication. These subfamily genes have, then, been amplified by 2R whole-genome duplication, followed by additional local duplications and gene loss prior to the divergence of land vertebrates and teleosts. This study delineates a possible evolutionary scenario for whole secretin-like peptide and receptor family members and may shed light on evolutionary mechanisms for expansion of a gene family with a large number of paralogs.
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