Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205
Introduction: The clinical use of kappa-opioid agonists, despite their lack of significant drug potential, is limited by the development of severe sedation, dysphoria, depression, and anhedonia. To this date, there are kappa-opioid receptor agonists lacking these side effec...
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doaj-b89487185e9748449c79f7468ff715bd2021-05-21T15:15:18ZengPensoft PublishersResearch Results in Pharmacology2658-381X2020-09-0163596510.3897/rrpharmacology.6.5455854558Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205Alexander A. Spasov0Edwin E. Zvartau1Olesya Iu. Grechko2Natalya V. Eliseeva3Yuliya V. Semenova4Olga A. Dravolina5Pavel M Vasiliev6Vera A. Anisimova7Volgograd State Medical University of the Ministry of Health of the Russian FederationI.P. Pavlov First St. Petersburg State Medical University of the Ministry of Health of the Russian FederationVolgograd State Medical University of the Ministry of Health of the Russian FederationVolgograd State Medical University of the Ministry of Health of the Russian FederationVolgograd State Medical University of the Ministry of Health of the Russian FederationI.P. Pavlov First St. Petersburg State Medical University of the Ministry of Health of the Russian FederationVolgograd State Medical University of the Ministry of Health of the Russian FederationSouthern Federal University Introduction: The clinical use of kappa-opioid agonists, despite their lack of significant drug potential, is limited by the development of severe sedation, dysphoria, depression, and anhedonia. To this date, there are kappa-opioid receptor agonists lacking these side effects due to the selective activation of intracellular signal transmission pathways without p38-MAPK-kinase activation. Materials and methods: We analyzed assessment of the docking energy of compound RU-1205 to the p38-MAPK active center by the method of similarity to SB203580. The study of possible aversive properties of RU-1205 (0.01–1 mg/kg s.c.) conducted in the tests of the intravenous self-administration and drug differentiation with butorphanol (0.01–0.3 mg/kg). The study of p38 MAPK-inhibitory activity was studied by the ability of RU-1205 to change the aversive properties of U50488 (10 mg/kg i.p.) compared to MAPK-kinase inhibitor SB203580 in the conditioned place avoidance test. Results: The spatial similarity coefficient of the RU-1205 molecule with SB203580 by the molecular conformation method was 1.14 (high similarity), and the docking energy was -8.7 Kcal/mol. RU-1205 did not possess any properties similar to those of butorphanol and did not demonstrate any primary reinforcing aversive properties in the development of intravenous self-administration reaction. Compound RU-1205 did not demonstrate any aversive properties in the conditioned place avoidance test, and reduced the development of aversion caused by U-50488, when they were used together. Discussion: The in silico analysis suggested that, in addition to agonism towards the kappa-opioid receptor, RU-1205 compound exhibits the properties of a p38 MAPK kinase inhibitor, which means it may have a double pharmacological activity. Conclusion: Kappa agonist – compound RU-1205 – is not a trigger of the development of behavioral patterns in animals corresponding to the development of addiction/dysphoria. The mechanism of such an activity may be associated with an inhibitory effect of compound RU-1205 on neuronal p38-MAPK-kinase. https://rrpharmacology.pensoft.net/article/54558/download/pdf/ |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Alexander A. Spasov Edwin E. Zvartau Olesya Iu. Grechko Natalya V. Eliseeva Yuliya V. Semenova Olga A. Dravolina Pavel M Vasiliev Vera A. Anisimova |
spellingShingle |
Alexander A. Spasov Edwin E. Zvartau Olesya Iu. Grechko Natalya V. Eliseeva Yuliya V. Semenova Olga A. Dravolina Pavel M Vasiliev Vera A. Anisimova Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 Research Results in Pharmacology |
author_facet |
Alexander A. Spasov Edwin E. Zvartau Olesya Iu. Grechko Natalya V. Eliseeva Yuliya V. Semenova Olga A. Dravolina Pavel M Vasiliev Vera A. Anisimova |
author_sort |
Alexander A. Spasov |
title |
Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 |
title_short |
Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 |
title_full |
Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 |
title_fullStr |
Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 |
title_full_unstemmed |
Study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound RU-1205 |
title_sort |
study of aversive and p38 mapk-inhibitory properties of kappa-agonist with analgesic activity – compound ru-1205 |
publisher |
Pensoft Publishers |
series |
Research Results in Pharmacology |
issn |
2658-381X |
publishDate |
2020-09-01 |
description |
Introduction: The clinical use of kappa-opioid agonists, despite their lack of significant drug potential, is limited by the development of severe sedation, dysphoria, depression, and anhedonia. To this date, there are kappa-opioid receptor agonists lacking these side effects due to the selective activation of intracellular signal transmission pathways without p38-MAPK-kinase activation. Materials and methods: We analyzed assessment of the docking energy of compound RU-1205 to the p38-MAPK active center by the method of similarity to SB203580. The study of possible aversive properties of RU-1205 (0.01–1 mg/kg s.c.) conducted in the tests of the intravenous self-administration and drug differentiation with butorphanol (0.01–0.3 mg/kg). The study of p38 MAPK-inhibitory activity was studied by the ability of RU-1205 to change the aversive properties of U50488 (10 mg/kg i.p.) compared to MAPK-kinase inhibitor SB203580 in the conditioned place avoidance test. Results: The spatial similarity coefficient of the RU-1205 molecule with SB203580 by the molecular conformation method was 1.14 (high similarity), and the docking energy was -8.7 Kcal/mol. RU-1205 did not possess any properties similar to those of butorphanol and did not demonstrate any primary reinforcing aversive properties in the development of intravenous self-administration reaction. Compound RU-1205 did not demonstrate any aversive properties in the conditioned place avoidance test, and reduced the development of aversion caused by U-50488, when they were used together. Discussion: The in silico analysis suggested that, in addition to agonism towards the kappa-opioid receptor, RU-1205 compound exhibits the properties of a p38 MAPK kinase inhibitor, which means it may have a double pharmacological activity. Conclusion: Kappa agonist – compound RU-1205 – is not a trigger of the development of behavioral patterns in animals corresponding to the development of addiction/dysphoria. The mechanism of such an activity may be associated with an inhibitory effect of compound RU-1205 on neuronal p38-MAPK-kinase. |
url |
https://rrpharmacology.pensoft.net/article/54558/download/pdf/ |
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