Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
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Target Concepts:
Gene/Protein
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Query: UNIPROT:P20366 (
substance P
)
21,176
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We have developed a non-peptide compound,
HSP
-117, antagonist of the
tachykinin
NK-1 receptor. Binding of 3H-
substance P
(SP) to the membranes of IM-9 cells was inhibited by the antagonists
HSP
-117 and CP-99,994, the inhibitory activity of
HSP
-117 being about 50-fold that of CP-99,994. The SP-induced firing responses of single neuron activity in slices of the nucleus tractus solitarius of ferrets were inhibited by 10 microM
HSP
-117. Intracerebroventricular injection of
HSP
-117 significantly inhibited retching and vomiting induced by copper sulphate and morphine and the inhibitory effect of
HSP
-117 on emesis was greater than that of CP-99,994. These results indicate that (1)
HSP
-117 is a potent anti-emetic agent, blocking NK-1 receptors in the nucleus tractus solitarius and (2) NK-1 receptors in the nucleus tractus solitarius play an important role in emesis induced by broad-spectrum emetic stimuli.
...
PMID:Anti-emetic effects of a novel NK-1 receptor antagonist HSP-117 in ferrets. 1021 84
Substance P
(SP) is a member of the
tachykinin
family of bioactive peptides and has highest affinity for the NK-1 receptor. We have developed the non-peptide compound
HSP
-117 as a selective antagonist of the NK-1 receptor. Binding of 3H-SP to the membranes of IM-9 cells was inhibited by the antagonists
HSP
-117 and CP-99,994, the inhibitory activity of
HSP
-117 being 50-fold that of CP-99,994. The SP-induced firing responses of single neuron activity in slices of the nucleus tractus solitarius of ferrets were inhibited by 10 microM
HSP
-117. Intracerebroventricular injection of
HSP
-117 significantly inhibited retching and vomiting induced by copper sulphate and morphine and the inhibitory effect of
HSP
-117 on emesis was greater than that of CP-99,994. Moreover, emesis induced by copper sulphate and morphine were inhibited by the microinjection of
HSP
-117 and CP-99,994 into the area postrema and by lesion of the area postrema. These results indicate that
HSP
-117 is a potent anti-emetic agent, blocking NK-1 receptors in the area postrema and that NK-1 receptors in the area postrema play an important role in emesis induced by broad-spectrum emetic stimuli.
...
PMID:[The role of tachykinin NK-1 receptors in emetic action in the area postrema of ferrets]. 1062 82
The role of
tachykinin
NK-1 receptors in the area postrema (AP) in emesis was examined in ferrets. Strong c-fos-like immunoreactivity was observed in the AP and nucleus tractus solitalius (NTS) in cisplatin (10 mg/kg, i.p.)-treated animals, but not in control animals. The number of the central emetogen morphine-induced vomits and retches was remarkably reduced (95%) and that of the peripheral emetogen copper sulphate-induced vomits was significantly (54%) reduced by AP lesion. Pretreatment with the
tachykinin
NK-1 receptor antagonists
HSP
-117 (1.0 microg) and CP-99,994 (7.5 microg) into the AP decreased the numbers of vomits and retches induced by morphine and copper sulphate. These results suggest that NK-1 receptors in the AP are involved in the mechanism of emesis induced by morphine and copper sulphate.
...
PMID:The role of tachykinin NK-1 receptors in the area postrema of ferrets in emesis. 1082 52
The effects of a novel
tachykinin
NK1-receptor antagonist
HSP
-117 [(2S,3S)-3-[(5-isopropyl-2,3-dihydrobenzofuran-7-yl)methyl]amino-2-phenylpiperidine dihydrochloride] on cisplatin-induced pica, i.e., the eating of nonnutritive substances such as kaolin were examined in rats.
HSP
-117 inhibited kaolin intake in a dose-dependent manner for 2 days. The 5-HT3-receptor antagonist ondansetron inhibited only on the first day, but not on the second day. These results indicate that the cisplatin-induced kaolin intake on the first day is related to both 5-HT3- and NK1 receptors, while only the NK1 receptor is involved on the second day. Thus, cisplatin-induced continuous pica in rats represents a useful model of not only acute but also delayed emesis.
...
PMID:Effects of HSP-117, a novel tachykinin NK1-receptor antagonist, on cisplatin-induced pica as a new evaluation of delayed emesis in rats. 1148 39
Solus par aqua (SPA) is a traditional health care therapy. Warm SPA may enhance immunity and cellular defense to protect body against diseases. The present study investigated whether the warm SPA could confer protection to neurogenic inflammation in rats. The rats were immersed in water where the body core temperatures were maintained at hyperthermia (41.5 degrees C) or normothermia (37 degrees C) for a period of 15min. After SPA for 1 or 6 days, neurogenic inflammation was induced by intravenous injection of capsaicin (90microg/kg) or
substance P
(SP; 3microg/kg). The plasma leakage and arterial pressures in rats after neurogenic inflammation were monitored. The extent of capsaicin- or SP-induced plasma leakage and hypotension was significantly attenuated in rats on day 1 after SPA hyperthermia. However, such resistance to neurogenic inflammation was not found on day 6 after hyperthermia. Western blotting analysis showed that the expression of heat shock protein 72 (
HSP
72) in the trachea on days 1 and 2 after hyperthermia was 9.61-fold and 6.66-fold, respectively, of that in normothermia. Afterwards, the hyperthermia-induced
HSP
72 upregulation gradually declined in a time-dependent manner. Thus, SPA hyperthermia may protect rats against neurogenic inflammation through modulation of
HSP
expression.
...
PMID:Warm SPA-induced hyperthermia confers protection to rats against airway inflammation evoked by capsaicin and substance P. 2013 90
