Study of μ- and δ-Opioid Activities in Agents with Various κ-Receptor Selectivity


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Abstract

A putative opioid agonist RU-1205 was ineffective within in vitro model of electrically induced contractions of rat ileum assessing the μ- and δ-opioid receptor pathways, while morphine inhibited these contractions in a dose-dependent and naloxone-reversible manners with EC50=2.6×10—7 M. In vivo experiments revealed no significant effects of RU-1205 on respiration and gastrointestinal tract contractile activity. In contrast, butorphanol decreased respiration rate by 25% (25-100 mg/kg) and slowed down the transit of labeled particles along the small intestine by 77.1% (1 mg/kg) and by 45.5% (10 mg/kg). Morphine-induced inhibition of peristalsis was dose-dependent with maximum effect (by 68.6%) observed in the dose of 10 mg/kg. It was concluded that the effects of RU-1205 are not related to activation μ- and δ-opioid receptors known to mediate the effects of non-selective opioid agonist morphine and agonist-antagonist butorphanol.

About the authors

O. Yu. Grechko

Volgograd State Medical University

Email: litvinov.volggmu@mail.ru
Russian Federation, Volgograd

R. A. Litvinov

Volgograd State Medical University

Author for correspondence.
Email: litvinov.volggmu@mail.ru
Russian Federation, Volgograd

A. A. Spasov

Volgograd State Medical University; Volgograd Medical Research Center

Email: litvinov.volggmu@mail.ru
Russian Federation, Volgograd; Volgograd

A. I. Rashchenko

Volgograd State Medical University

Email: litvinov.volggmu@mail.ru
Russian Federation, Volgograd

D. M. Shtareva

Volgograd State Medical University

Email: litvinov.volggmu@mail.ru
Russian Federation, Volgograd

V. A. Anisimova

Research Institute of Physical and Organic Chemistry, Southern Federal University

Email: litvinov.volggmu@mail.ru
Russian Federation, Rostov-on-Don

V. I. Minkin

Research Institute of Physical and Organic Chemistry, Southern Federal University

Email: litvinov.volggmu@mail.ru
Russian Federation, Rostov-on-Don


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