Literature DB >> 17286976

Molecular evolution of neuropeptide receptors with regard to maintaining high affinity to their authentic ligands.

Hyun Ju Cho1, Sujata Acharjee, Mi Jin Moon, Da Young Oh, Hubert Vaudry, Hyuk Bang Kwon, Jae Young Seong.   

Abstract

Recently, we cloned many of the bullfrog neuropeptide G protein-coupled receptors (GPCRs), including receptors for vasotocin (VT), mesotocin, gonadotropin-releasing hormone (GnRH), neurotensin, apelin, and metastin. Bullfrog GPCRs usually have high affinity for bullfrog ligands but relatively low affinity for mammalian ligands. Reciprocally, synthetic agonists and antagonists developed based upon mammalian ligands display lower affinity at bullfrog receptors. Studies using chimeric or domain-swapped receptors indicate that the motifs responsible for differential ligand selectivity usually reside within transmembrane domain 6 (TMD6)-extracellular loop 3 (ECL3)-transmembrane domain 7 (TMD7). Triple mutation of mammalian V1aR (Phe(6.51) to Tyr, Ile(6.53) to Thr, and Pro(7.33) to Thr) increases VT affinity but greatly reduces arginine vasopressin affinity. This binding profile is similar to that of bullfrog VT1R. Changing just three amino acids in the bullfrog GnRH receptor-1 (i.e. Ser-Gln-Ser in the ECL3) to those found in the type-I mammalian GnRH receptor (i.e. Ser-Glu-Pro) reverses GnRH selectivity. In conclusion, specific receptor motifs that govern ligand selectivity can be determined by comparative molecular analyses of GPCRs and their ligands. Such analysis provides clues for understanding how GPCRs maintain high affinity to their authentic ligands.

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Year:  2006        PMID: 17286976     DOI: 10.1016/j.ygcen.2006.12.013

Source DB:  PubMed          Journal:  Gen Comp Endocrinol        ISSN: 0016-6480            Impact factor:   2.822


  16 in total

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Review 4.  Regulatory decisions on endocrine disrupting chemicals should be based on the principles of endocrinology.

Authors:  Laura N Vandenberg; Theo Colborn; Tyrone B Hayes; Jerrold J Heindel; David R Jacobs; Duk-Hee Lee; John Peterson Myers; Toshi Shioda; Ana M Soto; Frederick S vom Saal; Wade V Welshons; R Thomas Zoeller
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5.  Effects of intracerebroventricular arginine vasotocin on a female amphibian proceptive behavior.

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6.  Molecular cloning, sequencing and phylogeny of vasotocin receptor genes in the air-breathing catfish Heteropneustes fossilis with sex dimorphic and seasonal variations in tissue expression.

Authors:  Arpana Rawat; Radha Chaube; Keerikkattil P Joy
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7.  Identification of antagonists to the vasotocin receptor sub-type 4 (VT4R) involved in stress by molecular modelling and verification using anterior pituitary cells.

Authors:  Srinivas Jayanthi; Seong Wook Kang; Daniel Bingham; Brian A Tessaro; Thallapuranam K Suresh Kumar; Wayne J Kuenzel
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8.  Molecular Coevolution of Neuropeptides Gonadotropin-Releasing Hormone and Kisspeptin with their Cognate G Protein-Coupled Receptors.

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Review 9.  Insights into the molecular evolution of oxytocin receptor ligand binding.

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10.  Structural and molecular conservation of glucagon-like Peptide-1 and its receptor confers selective ligand-receptor interaction.

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