Pharmacological profile of the cyclic nociceptin/orphanin FQ analogues c[Cys10,14]N/OFQ(1-14)NH2 and c[Nphe1,Cys10,14]N/OFQ(1-14)NH2

In this study we describe the activity of two cyclic nociceptin/orphanin FQ (N/OFQ) peptides; c[Cys(10,14)]N/OFQ(1-14)NH(2) (c[Cys(10,14)]) and its [Nphe(1)] derivative c[Nphe(1),Cys(10,14)]N/OFQ(1-14)NH(2) (c[Nphe(1),Cys(10,14)]) in native rat and mouse and recombinant human N/OFQ receptors (NOP)....

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Bibliographic Details
Published in:Naunyn-Schmiedeberg's archives of pharmacology 2003-12, Vol.368 (6), p.528-537
Main Authors: Kitayama, M, Barnes, T A, Carra, G, McDonald, J, Calo, G, Guerrini, R, Rowbotham, D J, Smith, G, Lambert, D G
Format: Article
Language:English
Subjects:
Animals
Binding, Competitive
Cell Membrane - metabolism
Cerebral Cortex - metabolism
CHO Cells
Colforsin - antagonists & inhibitors
Colforsin - pharmacology
Cricetinae
Cyclic AMP - biosynthesis
Cysteine - analogs & derivatives
Cysteine - metabolism
Cysteine - pharmacology
Dose-Response Relationship, Drug
Electric Stimulation
Female
GTP-Binding Proteins - metabolism
Male
Mice
Muscle Contraction - drug effects
Naloxone - pharmacology
Narcotic Antagonists
Nociceptin
Opioid Peptides - chemistry
Opioid Peptides - metabolism
Opioid Peptides - pharmacology
Phenylalanine - analogs & derivatives
Phenylalanine - metabolism
Phenylalanine - pharmacology
Radioligand Assay
Rats
Rats, Wistar
Receptors, Opioid - agonists
Receptors, Opioid - genetics
Receptors, Opioid - metabolism
Recombinant Proteins - agonists
Recombinant Proteins - antagonists & inhibitors
Recombinant Proteins - genetics
Recombinant Proteins - metabolism
Vas Deferens - drug effects
Vas Deferens - physiology
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Summary:In this study we describe the activity of two cyclic nociceptin/orphanin FQ (N/OFQ) peptides; c[Cys(10,14)]N/OFQ(1-14)NH(2) (c[Cys(10,14)]) and its [Nphe(1)] derivative c[Nphe(1),Cys(10,14)]N/OFQ(1-14)NH(2) (c[Nphe(1),Cys(10,14)]) in native rat and mouse and recombinant human N/OFQ receptors (NOP). Cyclisation may protect the peptide from metabolic degradation. In competition binding studies of rat, mouse and human NOP the following rank order pK(i) was obtained: N/OFQ(1-13)NH(2)(reference agonist)>N/OFQ=c[Cys(10,14)]>>c[Nphe(1)Cys(10,14)]. In GTPgamma(35)S studies of Chinese hamster ovary cells expressing human NOP (CHO(hNOP)) c[Cys(10,14)] (pEC(50) 8.29) and N/OFQ(1-13)NH(2) (pEC(50) 8.57) were full agonists whilst c[Nphe(1)Cys(10,14)] alone was inactive. Following 30 min pre-incubation c[Nphe(1)Cys(10,14)] competitively antagonised the effects of N/OFQ(1-13)NH(2) with a pA(2) and slope factor of 6.92 and 1.01 respectively. In cAMP assays c[Cys(10,14)] (pEC(50) 9.29, E(max) 102% inhibition of the forskolin stimulated response), N/OFQ(1-13)NH(2) (pEC(50) 10.16, E(max) 103% inhibition) and c[Nphe(1)Cys(10,14)] (~80% inhibition at 10 microM) displayed agonist activity. In the mouse vas deferens c[Cys(10,14)] (pEC(50) 6.82, E(max) 89% inhibition of electrically evoked contractions) and N/OFQ(1-13)NH(2) (pEC(50) 7.47, E(max) 93% inhibition) were full agonists whilst c[Nphe(1)Cys(10,14)] alone was inactive. c[Nphe(1)Cys(10,14)] (10 microM) competitively antagonised the effects of N/OFQ(1-13)NH(2) with a pK(B) of 5.66. In a crude attempt to assess metabolic stability, c[Cys(10,14)] was incubated with rat brain membranes and then the supernatant assayed for remaining peptide. Following 60 min incubation 64% of the 1 nM added peptide was metabolised (compared with 54% for N/OFQ-NH(2)). In summary, we report that c[Cys(10,14)] is a full agonist with a small reduction in potency but no improvement in stability whilst c[Nphe(1)Cys(10,14)] displays tissue (antagonist in the vas deferens) and assay (antagonist in the GTPgamma(35)S assay and agonist in cAMP assay) dependent activity.
ISSN:0028-1298
1432-1912
DOI:10.1007/s00210-003-0821-5