In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera

BACKGROUND: An important limiting factor in the development of centrally acting pharmaceuticals is the blood-brain barrier (BBB). Transport of therapeutic peptides through this highly protective physiological barrier remains a challenge for peptide drug delivery into the central nervous system (CNS)...

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Autores principales: Guillemyn, Karel, Kleczkowska, Patrycja, Novoa, Alexandre, Vandormael, Bart, Van den Eynde, Isabelle, Kosson, Piotr, Asim, Muhammad Faheem, Schiller, Peter W, Spetea, Mariana, Lipkowski, Andrzej W, Tourwé, Dirk, Ballet, Steven
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3284447/
https://www.ncbi.nlm.nih.gov/pubmed/22289619
http://dx.doi.org/10.1186/1756-6606-5-4
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author Guillemyn, Karel
Kleczkowska, Patrycja
Novoa, Alexandre
Vandormael, Bart
Van den Eynde, Isabelle
Kosson, Piotr
Asim, Muhammad Faheem
Schiller, Peter W
Spetea, Mariana
Lipkowski, Andrzej W
Tourwé, Dirk
Ballet, Steven
author_facet Guillemyn, Karel
Kleczkowska, Patrycja
Novoa, Alexandre
Vandormael, Bart
Van den Eynde, Isabelle
Kosson, Piotr
Asim, Muhammad Faheem
Schiller, Peter W
Spetea, Mariana
Lipkowski, Andrzej W
Tourwé, Dirk
Ballet, Steven
author_sort Guillemyn, Karel
collection PubMed
description BACKGROUND: An important limiting factor in the development of centrally acting pharmaceuticals is the blood-brain barrier (BBB). Transport of therapeutic peptides through this highly protective physiological barrier remains a challenge for peptide drug delivery into the central nervous system (CNS). Because the most common strategy to treat moderate to severe pain consists of the activation of opioid receptors in the brain, the development of active opioid peptide analogues as potential analgesics requires compounds with a high resistance to enzymatic degradation and an ability to cross the BBB. RESULTS: Herein we report that tetrapeptide analogues of the type H-Dmt(1)-Xxx(2)-Yyy(3)-Gly(4)-NH(2 )are transported into the brain after intravenous and subcutaneous administration and are able to activate the μ- and δ opioid receptors more efficiently and over longer periods of time than morphine. Using the hot water tail flick test as the animal model for antinociception, a comparison in potency is presented between a side chain conformationally constrained analogue containing the benzazepine ring (BVD03, Yyy(3): Aba), and a "ring opened" analogue (BVD02, Yyy(3): Phe). The results show that in addition to the increased lipophilicity through amide bond N-methylation, the conformational constraint introduced at the level of the Phe(3 )side chain causes a prolonged antinociception. Further replacement of NMe-D-Ala(2 )by D-Arg(2 )in the tetrapeptide sequence led to an improved potency as demonstrated by a higher and maintained antinociception for AN81 (Xxx(2): D-Arg) vs. BVD03 (Xxx(2): NMe-D-Ala). A daily injection of the studied opioid ligands over a time period of 5 days did however result in a substantial decrease in antinociception on the fifth day of the experiment. The compact opioid agonist - NK1 antagonist hybrid SBCHM01 could not circumvent opioid induced tolerance. CONCLUSIONS: We demonstrated that the introduction of a conformational constraint has an important impact on opioid receptor activation and subsequent antinociception in vivo. Further amino acid substitution allowed to identify AN81 as an opioid ligand able to access the CNS and induce antinociception at very low doses (0.1 mg/kg) over a time period up to 7 hours. However, tolerance became apparent after repetitive i.v. administration of the investigated tetrapeptides. This side effect was also observed with the dual opioid agonist-NK1 receptor antagonist SBCHM01.
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spelling pubmed-32844472012-02-25 In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera Guillemyn, Karel Kleczkowska, Patrycja Novoa, Alexandre Vandormael, Bart Van den Eynde, Isabelle Kosson, Piotr Asim, Muhammad Faheem Schiller, Peter W Spetea, Mariana Lipkowski, Andrzej W Tourwé, Dirk Ballet, Steven Mol Brain Research BACKGROUND: An important limiting factor in the development of centrally acting pharmaceuticals is the blood-brain barrier (BBB). Transport of therapeutic peptides through this highly protective physiological barrier remains a challenge for peptide drug delivery into the central nervous system (CNS). Because the most common strategy to treat moderate to severe pain consists of the activation of opioid receptors in the brain, the development of active opioid peptide analogues as potential analgesics requires compounds with a high resistance to enzymatic degradation and an ability to cross the BBB. RESULTS: Herein we report that tetrapeptide analogues of the type H-Dmt(1)-Xxx(2)-Yyy(3)-Gly(4)-NH(2 )are transported into the brain after intravenous and subcutaneous administration and are able to activate the μ- and δ opioid receptors more efficiently and over longer periods of time than morphine. Using the hot water tail flick test as the animal model for antinociception, a comparison in potency is presented between a side chain conformationally constrained analogue containing the benzazepine ring (BVD03, Yyy(3): Aba), and a "ring opened" analogue (BVD02, Yyy(3): Phe). The results show that in addition to the increased lipophilicity through amide bond N-methylation, the conformational constraint introduced at the level of the Phe(3 )side chain causes a prolonged antinociception. Further replacement of NMe-D-Ala(2 )by D-Arg(2 )in the tetrapeptide sequence led to an improved potency as demonstrated by a higher and maintained antinociception for AN81 (Xxx(2): D-Arg) vs. BVD03 (Xxx(2): NMe-D-Ala). A daily injection of the studied opioid ligands over a time period of 5 days did however result in a substantial decrease in antinociception on the fifth day of the experiment. The compact opioid agonist - NK1 antagonist hybrid SBCHM01 could not circumvent opioid induced tolerance. CONCLUSIONS: We demonstrated that the introduction of a conformational constraint has an important impact on opioid receptor activation and subsequent antinociception in vivo. Further amino acid substitution allowed to identify AN81 as an opioid ligand able to access the CNS and induce antinociception at very low doses (0.1 mg/kg) over a time period up to 7 hours. However, tolerance became apparent after repetitive i.v. administration of the investigated tetrapeptides. This side effect was also observed with the dual opioid agonist-NK1 receptor antagonist SBCHM01. BioMed Central 2012-01-30 /pmc/articles/PMC3284447/ /pubmed/22289619 http://dx.doi.org/10.1186/1756-6606-5-4 Text en Copyright ©2012 Guillemyn et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Guillemyn, Karel
Kleczkowska, Patrycja
Novoa, Alexandre
Vandormael, Bart
Van den Eynde, Isabelle
Kosson, Piotr
Asim, Muhammad Faheem
Schiller, Peter W
Spetea, Mariana
Lipkowski, Andrzej W
Tourwé, Dirk
Ballet, Steven
In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title_full In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title_fullStr In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title_full_unstemmed In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title_short In vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
title_sort in vivo antinociception of potent mu opioid agonist tetrapeptide analogues and comparison with a compact opioid agonist - neurokinin 1 receptor antagonist chimera
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3284447/
https://www.ncbi.nlm.nih.gov/pubmed/22289619
http://dx.doi.org/10.1186/1756-6606-5-4
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