Non-peptide ligands in the characterization of peptide receptors at the interface between neuroendocrine and mental diseases  被引量：2

作　　者：Margit Pissarek Ulrich Disko 

机构地区：[1]IBG-3, Institute of Bio- and Geosciences, Research Centre Jülich, Jülich, Germany [2]INM-5 Nuclear Chemistry, Institute of Neuroscience and Medicine, Jülich, Germany

出　　处：《World Journal of Neuroscience》2013年第2期100-125,共26页神经科学国际期刊（英文）

摘　　要：Hypothalamic receptors for neuropeptide Y, melaninconcentrating hormone, melanocortins and orexins/ hypocretins as well as for the downstream signaling corticotrophic factor have been discussed broadly for their influence on food intake and reward but also on several psychiatric disorders. For the development of non-peptide ligands for the in vivo detection of alterations in density and affinity of such G-protein coupled (GPCRs) peptide receptors the requirements to affinity and pharmacokinetics have been shifted to thresholds markedly distict from classical GPCRs to dissociation constants ported originally as potential therapeutics in the treatment of obesity among which some are suitable candidates for labeling as PET or SPECT-tracers providing receptor affinities even below 0.1 nM. These could be unique tools not only for better understanding of the mechanism of obesity but also for investigations of extrahypothalamic role of “feeding receptors” at the interface between neuroendocrine and mental diseases.Hypothalamic receptors for neuropeptide Y, melaninconcentrating hormone, melanocortins and orexins/ hypocretins as well as for the downstream signaling corticotrophic factor have been discussed broadly for their influence on food intake and reward but also on several psychiatric disorders. For the development of non-peptide ligands for the in vivo detection of alterations in density and affinity of such G-protein coupled (GPCRs) peptide receptors the requirements to affinity and pharmacokinetics have been shifted to thresholds markedly distict from classical GPCRs to dissociation constants ported originally as potential therapeutics in the treatment of obesity among which some are suitable candidates for labeling as PET or SPECT-tracers providing receptor affinities even below 0.1 nM. These could be unique tools not only for better understanding of the mechanism of obesity but also for investigations of extrahypothalamic role of “feeding receptors” at the interface between neuroendocrine and mental diseases.

关 键 词：FEEDING Receptor HYPOTHALAMUS NEUROPEPTIDE NON-PEPTIDE ANTAGONIST PET SPECT 

分 类 号：R73[医药卫生—肿瘤]