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Inverse agonism at neurotensin receptors NTS1 and NTS2

机译:神经狭窄受体NTS1和NTS2的反向激动

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Neurotensin (NT) is a peptide expressed in the brain and small intestines. Its central effects include analgesia, inhibition of food intake, modulation of central dopaminergic systems, and modulation of pituitary hormones secretion. In the gut, neurotensin is released upon food ingestion to regulate digestive functions. In addition, the peptide acts as a trophic factor on human colon, pancreatic, prostate, and lung cancer cell lines. Thus, neurotensin receptors represent interesting targets for the treatment of pain, obesity, schizophrenia, and cancer. Two neurotensin receptors, NTS1 and NTS2, that belong to the family of G protein-coupled receptors have been identified. A nonpeptide antagonist with selectivity for the NTS 1, SR 48692, has been characterized. Recent mutagenesis and modeling studies allowed us to map agonist and antagonist binding sites in the NTS1 and to identify extracellular and transmembrane (TM) residues involved in receptor activation. In particular, we identified a transmembrane residue whose mutation confers constitutive activity to the NTS1 and reveals inverse agonist properties of SR 48692. Quite recently, we demonstrated that the human NTS2 is constitutively active and we characterized agonist, inverse agonist, and neutral antagonist ligands at this receptor. These results and then- implications are the focus of the present paper.
机译:神经调节素(NT)是在脑和小肠中表达的肽。其集中效应包括镇痛,抑制食物摄入量,调节中央多巴胺能系统,以及垂体激素分泌的调节。在肠道中,神经调素在食物摄取后释放以调节消化功能。此外,肽作为人结肠,胰腺,前列腺和肺癌细胞系的营养因子。因此,神经调节素受体代表了治疗疼痛,肥胖,精神分裂症和癌症的有趣靶标。已经鉴定了属于G蛋白偶联受体系列的两种神经调度素受体,NTS1和NTS2。已经表征了具有NTS 1,SR 48692的选择性的非肽拮抗剂。最近的诱变和建模研究使我们可以在NTS1中映射激动剂和拮抗剂结合位点,并鉴定参与受体活化的细胞外和跨膜(TM)残基。特别地,我们鉴定了一种跨膜残基,其突变将本构成的活性赋予NTS1,并揭示了SR 48692的逆激动剂性质。最近,我们证明了人体NTS2组成型活性,并且我们表征着激动剂,逆激动剂和中性拮抗剂配体这个受体。这些结果和目的是本文的重点。

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