Literature DB >> 16515546

Big dynorphin as a putative endogenous ligand for the kappa-opioid receptor.

Florence Merg1, Dominique Filliol, Ivan Usynin, Igor Bazov, Niklas Bark, Yasmin L Hurd, Tatjana Yakovleva, Brigitte L Kieffer, Georgy Bakalkin.   

Abstract

The diversity of peptide ligands for a particular receptor may provide a greater dynamic range of functional responses, while maintaining selectivity in receptor activation. Dynorphin A (Dyn A), and dynorphin B (Dyn B) are endogenous opioid peptides that activate the kappa-opioid receptor (KOR). Here, we characterized interactions of big dynorphin (Big Dyn), a 32-amino acid prodynorphin-derived peptide consisting of Dyn A and Dyn B, with human KOR, mu- (hMOR) and delta- (hDOR) opioid receptors and opioid receptor-like receptor 1 (hORL1) expressed in cells transfected with respective cDNA. Big Dyn and Dyn A demonstrated roughly similar affinity for binding to hKOR that was higher than that of Dyn B. Dyn A was more selective for hKOR over hMOR, hDOR and hORL1 than Big Dyn, while Dyn B demonstrated low selectivity. In contrast, Big Dyn activated G proteins through KOR with much greater potency, efficacy and selectivity than other dynorphins. There was no correlation between the rank order of the potency for the KOR-mediated activation of G proteins and the binding affinity of dynorphins for KOR. The rank of the selectivity for the activation of G proteins through hKOR and of the binding to this receptor also differed. Immunoreactive Big Dyn was detected using the combination of radioimmunoassay (RIA) and HPLC in the human nucleus accumbens, caudate nucleus, hippocampus and cerebrospinal fluid (CSF) with the ratio of Big Dyn and Dyn B being approximately 1:3. The presence in the brain implies that Big Dyn, along with other dynorphins, is processed from prodynorphin and secreted from neurons. Collectively, the high potency and efficacy and the relative abundance suggest that Big Dyn may play a role in the KOR-mediated activation of G proteins.

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Year:  2006        PMID: 16515546     DOI: 10.1111/j.1471-4159.2006.03732.x

Source DB:  PubMed          Journal:  J Neurochem        ISSN: 0022-3042            Impact factor:   5.372


  28 in total

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Journal:  Int J Clin Exp Med       Date:  2014-12-15

Review 3.  Endogenous opiates and behavior: 2006.

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Journal:  Peptides       Date:  2007-09-11       Impact factor: 3.750

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5.  Prodynorphin gene promoter polymorphism and temporal lobe epilepsy: A meta-analysis.

Authors:  Na Zhang; Tao-Hui Ouyang; Qing Zhou; Hui-Cong Kang; Sui-Qiang Zhu
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Review 6.  Salvinorin A analogs and other κ-opioid receptor compounds as treatments for cocaine abuse.

Authors:  Bronwyn M Kivell; Amy W M Ewald; Thomas E Prisinzano
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Review 7.  Targeting dynorphin/kappa opioid receptor systems to treat alcohol abuse and dependence.

Authors:  Brendan M Walker; Glenn R Valdez; Jay P McLaughlin; Georgy Bakalkin
Journal:  Alcohol       Date:  2012-03-27       Impact factor: 2.405

8.  Alanine scan of the opioid peptide dynorphin B amide.

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Journal:  Biopolymers       Date:  2017-09       Impact factor: 2.505

9.  Dynorphin opioid peptides enhance acid-sensing ion channel 1a activity and acidosis-induced neuronal death.

Authors:  Thomas W Sherwood; Candice C Askwith
Journal:  J Neurosci       Date:  2009-11-11       Impact factor: 6.167

10.  Asymmetry of the endogenous opioid system in the human anterior cingulate: a putative molecular basis for lateralization of emotions and pain.

Authors:  Hiroyuki Watanabe; Sylvia Fitting; Muhammad Z Hussain; Olga Kononenko; Anna Iatsyshyna; Takashi Yoshitake; Jan Kehr; Kanar Alkass; Henrik Druid; Henrik Wadensten; Per E Andren; Ingrid Nylander; Douglas H Wedell; Oleg Krishtal; Kurt F Hauser; Fred Nyberg; Victor M Karpyak; Tatjana Yakovleva; Georgy Bakalkin
Journal:  Cereb Cortex       Date:  2013-08-19       Impact factor: 5.357

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