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Target Concepts:
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Query: UMLS:C0344307 (
analgesia
)
28,200
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The effects of Prolyl-leucyl-glycinamide (
PLG
, MIF-1) and the exogenous opiate antagonist naloxone, on aggressive interactions and defeat-induced
analgesia
were examined in male mice. Both substances reduced the number of bites required to obtain defeat in subordinate mice during aggressive encounters as well as blocking the subsequent defeat-induced
analgesia
. These results suggest that MIF-1 may function as an endogenous opioid antagonist and have an inhibitory influence on aggression.
...
PMID:Prolyl-leucyl-glycinamide reduces aggression and blocks defeat-induced opioid analgesia in mice. 286 8
The effects of i.c.v. administration of the peptide FMRFamide (Phe-Met-Arg-Phe-NH2), as well as i.p. injections of
PLG
(Pro-Leu-Gly-NH2) and the opiate antagonist, naloxone, on immobilization-induced
analgesia
and locomotor activity were examined in CF-1 and C57BL strains of mice. Both naloxone (1.0 mg/kg) and FMRFamide (0.10-1.0 microgram) blocked the experimentally induced
analgesia
and activity, whereas
PLG
(0.10-10 mg/kg) suppressed only
analgesia
. These results indicate that FMRFamide (or FMRFamide-like neuropeptides) and
PLG
may function as differential antagonists of the behavioral and physiological consequences of endogenous opioid activation.
...
PMID:Inhibitory influences of FMRFamide and PLG on stress-induced opioid analgesia and activity. 287 3
The effects of prolyl-leucyl-glycinamide (MIF-1,
PLG
), tyrosine-prolyl-leucyl-glycinamide (Tyr-MIF-1, YPLG) and the exogenous opiate antagonist, naloxone, on aggressive interactions and defeat-induced
analgesia
were examined in male mice. All three substances reduced the number of bites required to obtain defeat in subordinate mice during aggressive encounters, as well as blocking subsequent defeat-induced
analgesia
. Tyr-MIF-1 had significantly greater inhibitory effects than MIF. These results suggest that both MIF and Tyr-MIF-1 may function as endogenous opioid antagonists and have inhibitory influences on aggression, with the antagonistic effects of Tyr-MIF-1 being more potent than those of MIF-1.
...
PMID:Inhibitory influences of MIF-1 (PLG) and Tyr-MIF-1 (YPLG) on aggression and defeat-induced analgesia in mice. 288 93
The effects of prolyl-leucyl-glycinamide (MIF-1,
PLG
), tyrosine-prolyl-leucyl-glycinamide (Tyr-MIF-1, YPLG) and naloxone on morphine and warm and cold stress-induced increases in the latency of the thermal (40 degrees C hot plate) avoidance behaviors of the terrestrial snail, Cepaea nemoralis, were examined. All three substances blocked the morphine- and warm stress-induced opioid
analgesia
, while having no effects on non-opioid cold stress-induced
analgesia
. Tyr-MIF-1 had a significantly greater inhibitory effect than MIF-1. These results indicate that MIF-1 and Tyr-MIF-1 antagonize the antinociceptive effects of exogenous opiates and opioid-mediated
analgesia
in snails in a manner analogous to that described for mammals. This raises the possibility of an evolutionary conservation of functional opioid antagonists.
...
PMID:MIF-1 and Tyr-MIF-1 antagonize morphine and opioid but not non-opioid stress-induced analgesia in the snail, Cepaea nemoralis. 288 31
Oral naltrexone, a nonselective opioid antagonist, is approved for the treatment of alcohol and opioid dependence. However, the efficacy of oral naltrexone is limited by poor patient compliance. To overcome this limitation, attempts have been made to develop an injectable extended-release formulation of naltrexone, including encapsulation into biodegradable polymer microspheres (e.g. Medisorb Naltrexone, Vivitrex (naltrexone long acting injection)). In 1980, NIDA established development goals that they considered optimal for an extended-release formulation. At Alkermes, different formulations were tested with in vitro assays and in vivo models to select a lead formulation. Pharmacokinetic studies in rats confirmed that the principle formulation produced stable, pharmacologically relevant plasma levels of naltrexone for approximately one month following a single injection. The pharmacodynamic effects (antagonism of morphine
analgesia
) of extended-release naltrexone corresponded well with the pharmacokinetic profile from the same animals. While brain mu-opioid receptor density was found to increase over time in these rats, it did not appear to affect the ability of naltrexone to suppress morphine
analgesia
. Finally the pharmacokinetic profile of extended-release naltrexone in monkeys confirmed long duration of elevated plasma concentrations of naltrexone. Both naltrexone and the
PLG
polymer matrix in which it is encapsulated are well tolerated. Clinical trials of Vivitrex are currently ongoing in alcohol dependent patients.
...
PMID:The preclinical development of Medisorb Naltrexone, a once a month long acting injection, for the treatment of alcohol dependence. 1556 5
