Evolutionary expression of glucose-dependent-insulinotropic polypeptide (GIP)
- Authors
- Musson, M.C., Jepeal, L.I., Finnerty, J.R., and Wolfe, M.M.
- ID
- ZDB-PUB-110713-1
- Date
- 2011
- Source
- Regulatory peptides 171: 26-34 (Journal)
- Registered Authors
- Keywords
- enterionsular axis, glucose-dependent insulinotropic polypeptide, incretin, phylogeny
- MeSH Terms
-
- Animals
- Chickens/genetics
- Evolution, Molecular*
- Gastric Inhibitory Polypeptide/genetics*
- Gastric Inhibitory Polypeptide/metabolism
- Gene Expression
- Insulin/genetics*
- Insulin/metabolism
- Intestines/metabolism
- Mice
- Pancreas/metabolism
- Petromyzon/genetics*
- Petromyzon/metabolism
- Phylogeny
- Proglucagon/genetics*
- Xenopus laevis/genetics
- Xenopus laevis/metabolism
- Zebrafish/genetics*
- Zebrafish/metabolism
- PubMed
- 21723886 Full text @ Regul. Pept.
Glucose-dependent insulinotropic polypeptide (GIP) is a mammalian incretin hormone released into the circulation following nutrient ingestion. We examined the functional evolution of GIP and its relationship with insulin to delineate their respective roles in promoting nutrient efficiency. Expression patterns were examined in the sea lamprey (Petromyzon marinus), a basal vertebrate lacking a distinct pancreas, and in the zebrafish, Xenopus laevis, chicken, and mouse, organisms possessing extraintestinal pancreata. Although sea lamprey genomic analysis predicted a potential GIP-like gene, transcripts were not detected, and insulin expression was confined to the caudal pancreatic bud. GIP was detected in both the intestine and pancreas of the zebrafish and X. laevis. In contrast, GIP and insulin expression were limited to the intestine and pancreas, respectively, in chicken and mouse. Phylogenetic analysis of the glucagon-like ligands suggested proglucagon as the common ancestor, supporting the theory that GIP arose as a gene duplication of proglucagon. Insulin-secreting cells in the sea lamprey intestine may have obviated the need for an enteroinsular axis, and zebrafish may represent an evolutionary transition where GIP does not yet function as an incretin hormone. These observations are consistent with the hypothesis that GIP and insulin influence survival advantage by enhancing the efficiency of nutrient absorption and energy storage.