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Optimized GIP analogs promote body weight lowering in mice through GIPR agonism not antagonism.

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  • Additional Information
    • Publication Information:
      Elsevier Science Bv
    • Publication Date:
      2019
    • Collection:
      PuSH - Publikationsserver des Helmholtz Zentrums München
    • Abstract:
      Objective: Structurally-improved GIP analogs were developed to determine precisely whether GIP receptor (GIPR) agonism or antagonism lowers body weight in obese mice.Methods: A series of peptide-based GIP analogs, including structurally diverse agonists and a long-acting antagonist, were generated and characterized in vitro using functional assays in cell systems overexpressing human and mouse derived receptors. These analogs were characterized in vivo in DIO mice following acute dosing for effects on glycemic control, and following chronic dosing for effects on body weight and food intake. Pair-feeding studies and indirect calorimetry were used to survey the mechanism for body weight lowering. Congenital Gipr-/- and Glp1r-/- DIO mice were used to investigate the selectivity of the agonists and to ascribe the pharmacology to effects mediated by the GIPR.Results: Non-acylated, Aib2 substituted analogs derived from human GIP sequence showed full in vitro potency at human GIPR and subtly reduced in vitro potency at mouse GIPR without cross-reactivity at GLP-1R. These GIPR agonists lowered acute blood glucose in wild-type and Glp1r-/- mice, and this effect was absent in Gipr-/- mice, which confirmed selectivity towards GIPR. Chronic treatment of DIO mice resulted in modest yet consistent, dose-dependent decreased body weight across many studies with diverse analogs. The mechanism for body weight lowering is due to reductions in food intake, not energy expenditure, as suggested by pair-feeding studies and indirect calorimetry assessment. The weight lowering effect was preserved in DIO Glp-1r-/- mice and absent in DIO Gipr-/- mice. The body weight lowering efficacy of GIPR agonists was enhanced with analogs that exhibit higher mouse GIPR potency, with increased frequency of administration, and with fatty-acylated peptides of extended duration of action. Additionally, a fatty-acylated, N-terminally truncated GIP analog was shown to have high in vitro antagonism potency for human and mouse GIPR without cross-reactive ...
    • File Description:
      application/pdf
    • ISSN:
      2212-8778
    • Relation:
      info:eu-repo/semantics/altIdentifier/pmid/30578168; info:eu-repo/semantics/altIdentifier/wos/WOS:000456819100005; info:eu-repo/semantics/altIdentifier/isbn/2212-8778; info:eu-repo/semanti; https://push-zb.helmholtz-muenchen.de/frontdoor.php?source_opus=55037; urn:isbn:2212-8778; urn:issn:2212-8778
    • Accession Number:
      10.1016/j.molmet.2018.12.001
    • Online Access:
      https://push-zb.helmholtz-muenchen.de/frontdoor.php?source_opus=55037
      https://doi.org/10.1016/j.molmet.2018.12.001
    • Rights:
      info:eu-repo/semantics/openAccess
    • Accession Number:
      edsbas.B1DA8F11