ACTA FAC
MED NAISS 2014;31(1):41-49|
ACTA FAC
MED NAISS 2014;31(1):41-49 |
Original article
UDC:615.212
DOI:10.2478/afmnai-2014-0004
Involvement of the Vanilloid Receptor 1 in the Mechanisms of Analgesic Effect of Amizonum
Oleh Yadlovskyi, Tatiana Bukhtiarova, Lyudmila Bobkova, Irina Tatianshenko, Igor Monchak, Andrew Khayrulin
State Institution «Institute of pharamcology
and Toxicology of NAMS of Ukraine», Kiev, Ukraine
summary
The study of features of pharmacodynamics of a new analgesic is an important and
urgent task of modern pharmacology. These data allow us to clarify the nosology
for application of an analgesic and to create a theoretical background to
optimize its use. An effect mediated by the transient receptor potential cation
channel, subfamily V, member 1 (TRPV1) activation can also be an effective
mechanism of the analgesic action. We evaluated the possibility of TRPV1
participation in implementation of the analgesic effect with the antiviral
action of amizonum during the experiment. It is known that amino acids Tyr511
and Ser512 are the main components of the active site of TRPV1. In this
connection, dipeptide Tyr-Ser has been completely synthesized as a model of the
active site of TRPV1. In the experiment model this was shown, using the
spectrophotometric method, with the formation of the “capsaicin - Tyr-Ser”
intermolecular complex at the level of the stability constant Kkor=0.998 and
Kr=0.3•10-4 L/mol and the “amizonum - Tyr-Ser” weak intermolecular complex
Kr=0.05•104 L/mol; Kkor= 0.995, respectively. The data verification was carried
out in experiments in vitro (isolated rat-portal vein) and in vivo (Tail-flick
model), with the TRPV1 agonist. It was shown that the amplitude of smooth muscle
(SM) contraction of the portal vein at a capsaicin concentration 0.1 µmol/L, 0.5
µmol/L capsazepine, and 1.0 µmol/L amizonum was +30.3±5.3%, -3.2± 2.7% and
+7.1±3.2% from initial level, respectivelly. In a combined application of
amizonum with capsaicin or capsazepine, the amplitude of contraction of the SM
portal vein was 20.1± 1.3% and -3.0±1.4%, respectively. This indicates the
absence of action of amizonum under combined use of capsaicinoids. The
Tail-flick model showed atypical potentiation of the amizonum antinociception
with the use of capsaicin. The obtained data suggest the low probability of the
participation of TRPV1 in the implementation of the antinociceptive action of
amizonum.
Key words: amizonum, capsaicin, capsazepine, dipeptide Tyr-Ser (Tyr-Ser), TRPV1