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Query: UNIPROT:P20366 (
substance P
)
21,176
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Following the recent discovery of a new
substance P
(SP) competitive pancreatic acini cell receptor antagonist containing a reduced peptide bond in place of the C-terminal peptide bond, a new series of full chain and short chain (heptapeptide and hexapeptide)
substance P
analogues have been prepared in which one of the C-terminal-region peptide bonds has been replaced by CH2NH or CH2O groups. They were compared for their ability to recognize
NK1
and/or NK2
tachykinin
receptor binding sites on guinea pig ileum and rat duodenum smooth muscle preparations, respectively. It was found that all full sequence SP pseudopeptides were agonists with much reduced bioactivity in both tested systems and, in addition, [Gly9 psi(CH2NH)Leu10,Leu11]SP was found to be a relatively selective agonist for
NK1
binding sites. Substitution of leucine at position 11 of SP heptapseudopeptides with phenylalanine generated a pseudopeptide with weak agonist activity when Gln at position 5 was replaced by D-Phe, or antagonists when this residue was replaced by D-Nal or D-Cpa. [Leu10 psi(CH2NH)Leu11]SP-(6-11) with Gln at position 6 substituted by D-Phe was a relatively stronger antagonist in both assay systems. These results suggest that, as with several other peptide systems of late, manipulation of the peptide bonds in SP can produce receptor antagonists which in some cases approach the potency of the classic spantide series and, furthermore, that the approach might be used to induce NK receptor specificity in both agonist and antagonist analogs.
...
PMID:New reduced peptide bond substance P agonists and antagonists: effects on smooth muscle contraction. 172 44
The contractile effect of
substance P
,
neurokinin A
, receptor selective agonists for
tachykinin
receptors and NK2
tachykinin
receptor antagonists was investigated in mucosa-free circular strips of the human isolated colon.
Neurokinin A
and
substance P
produced concentration-dependent contractions which approached 80-90% of the maximal response to carbachol.
Neurokinin A
was about 370 times more potent than
substance P
. The action of
neurokinin A
and
substance P
was not modified by peptidase inhibitors (bestatin, captopril and thiorphan, 1 microM each). The NK2 receptor selective agonist, [beta-Ala8]
neurokinin A
-(4-10) closely mimicked the response to
neurokinin A
while
NK1
and NK3 receptor selective agonists were active only at microM concentrations. The pseudopeptide, MDL 28,564, which is one of the most selective NK2 ligands available, behaved as a full agonist. Responses to [beta-Ala8]
neurokinin A
were antagonized by NK2 receptor selective antagonists, with the rank order of potency MEN 10,376 greater than L 659,877 much greater than R 396. These data indicate that NK2
tachykinin
receptors play a dominant role in determining the contraction of the circular muscle of the human colon to peptides of this family. The NK2 receptor subtype responsible for this effect belongs to the same subtype (NK2A) previously identified in the rabbit pulmonary artery and guinea-pig bronchi.
...
PMID:NK2 tachykinin receptors and contraction of circular muscle of the human colon: characterization of the NK2 receptor subtype. 172 45
This study examined the influence of cytokines on
substance P
(SP) receptors (
NK1
subtype) in the human astrocytoma cell line UC11. Following trypsinization and passage, the density of SP receptors in these cells was rather low but gradually increased several fold over the course of a few days in culture. Frequent replacement of the growth medium enhanced the density of receptors even more, suggesting that growth factors in the culture medium may determine the levels of receptor. Exposure of the cells to sub-nanomolar concentrations of tumor necrosis factor (TNF alpha) or interleukin-1 beta (IL1 beta), but not interleukin-2 or interleukin-6, decreased the density of SP receptors. This was accompanied by a decrease in the ability of SP to stimulate inositolphosphate formation. The ability of histamine to activate inositolphosphate formation was not influenced by the cytokines. The decrease in SP receptor density was readily reversible on washout of the cytokines. The EC50 for TNF alpha was approximately 0.5 ng/ml, the EC50 for IL1 beta was approximately 0.1 ng/ml. Radioligand binding studies with [125I]TNF alpha indicated the presence of a low density of high affinity binding sites for this ligand: Kd = 2.5 +/- 0.6 ng/ml, Bmax = 14.8 +/- 2.7 fmol bound/mg protein (assuming trimeric form of ligand bound). The most likely explanation for the cytokine effect is an inhibition of the synthesis of new receptors.
...
PMID:Tumor necrosis factor and interleukin-1 down-regulate receptors for substance P in human astrocytoma cells. 172 42
The affinities of various
substance P
agonists and antagonists for
NK1
receptors in rat and guinea-pig tissues were compared. Striking species differences were observed. Both septide and [D-Pro4,D-Trp7,9]SP-(4-11) possessed much higher affinity for sites in the guinea-pig (brain and ileum) than for sites in the rat brain. These results could be explained by differences in the structure of the
NK1
receptor according to the species, although the existence of various subtypes of
NK1
binding sites in the two species cannot be excluded.
...
PMID:Species differences between [3H] substance P binding in rat and guinea-pig shown by the use of peptide agonists and antagonists. 172 51
The NK3 agonist, senktide, induced a potent contraction of rat uterus in the presence of tetrodotoxin, atropine and indomethacin, or the
tachykinin
receptor antagonists L-659877 and [D-Pro4,D-Trp7,9,10]
substance P
(4-11). Additional contractile and radioligand binding studies with receptor selective agonists and antagonists confirmed the presence of NK3 receptors and also revealed the presence of
NK1
and NK2 receptors. The rat uterus is the second peripheral tissue in which a post-synaptic, non-neuronal NK3 receptor has been identified.
...
PMID:The presence of NK3 tachykinin receptors on rat uterus. 172 57
Recent in vitro studies have shown that the dose-response curve of
substance P
on [3H]protein secretion from rat parotid glands is biphasic. Such a response could result either from the activation of
tachykinin
receptors or from the amphiphilic character of
substance P
, since it has previously been shown that the N-terminal part of
substance P
may play an important role in the activation of phosphoinositides in rat parotid glands. To investigate these possibilities, we studied the effects of selective
NK1
, NK2, NK3 receptor agonists and C-terminal fragments of
substance P
and
neurokinin A
on protein secretion from rat parotid lobules. The poor activity of NK2 (
neurokinin A
-(4-10) and [beta-Ala8]
neurokinin A
-(4-10)) as well as of NK3 ([MePhe7]neurokinin B) selective agonists allowed us to rule out a possible involvement of NK2 and NK3 receptors in the parotid gland secretory process. Conversely, the selective
NK1
receptor agonist, [Sar9,Met(O2)11]
substance P
, reproduced the biphasic dose-response curve for [3H]protein secretion typical of native
substance P
. However, a biphasic response was not observed with peptides deprived of the N-terminal moiety of
substance P
, such as
substance P
-(4-11) or [AcArg6,Sar9,Met(O2)11]
substance P
-(6-11). Our data therefore indicate that the [3H]protein secretion obtained with
substance P
results from the activation of
NK1
receptors. Moreover, our data suggest that the N-terminal tripeptide of
substance P
is also active, and could stimulate different phospholipases either by acting through a second functional site on the
NK1
receptor or by directly activating G-proteins.
...
PMID:Involvement of NK1 receptors and importance of the N-terminal sequence of substance P in the stimulation of protein secretion in rat parotid glands. 172 89
The
neurokinin A
analogue, MDL 28,564 (Asp-Ser-Phe-Val-Gly-Leu-CH2NH-Leu-NH2), inhibited 125I-NKA binding to hamster urinary bladder NK2 receptors with a KI of 130 nM. For rat submaxillary gland
NK1
receptors and cerebral cortical NK3 receptors, the KI's for MDL 28,564 were greater than 250 microM and greater than 500 microM, respectively. MDL 28,564 did not relax dog carotid artery (
NK1
tissue) or contract rat portal vein (NK3 tissue). In guinea-pig trachea tissues, MDL 28,564 stimulated phosphatidylinositol turnover and induced contraction with maximum effects similar to those of
neurokinin A
. In hamster urinary bladder tissue, MDL 28,564 stimulated phosphatidylinositol turnover with maximum effect only 10% of that of
neurokinin A
, did not produce sustained contraction itself and antagonized NKA-induced contraction. MDL 28,564 also produced full contraction in rabbit pulmonary artery (NK2 tissue) but was inactive in rat vas deferens (NK2 tissue). These data with MDL 28,564 are consistent with the NK2 receptors in guinea-pig trachea and rabbit pulmonary artery being different from those in hamster urinary bladder and rat vas deferens.
...
PMID:[Leu9 psi(CH2NH)Leu10]-neurokinin A (4-10) (MDL 28,564) distinguishes tissue tachykinin peptide NK2 receptors. 217 Jul 88
To test the effects on gastric acid secretion and gastric emptying of non-mammalian (eledoisin, physalaemin, kassinin), mammalian (
substance P
.
neurokinin A
, neurokinin B) and synthetic tachykinins (septide, senktide), intracerebroventricular injections of these peptides were given to conscious pylorus-ligated rats (gastric secretory study) or to animals fed with a phenol red meal (gastric emptying study). The tachykinins able to cause central inhibition of acid output were those active on NK2 and NK3 receptors (eledoisin, kassinin,
neurokinin A
, neurokinin B and senktide). Tachykinins active on
NK1
receptors (
substance P
. physalaemin and septide) were devoid of this activity. The most potent inhibitor was the synthetic NK3 agonist, senktide. All tested natural tachykinins significantly inhibited gastric emptying, the most potent being those active on NK2 receptors. Septide, the synthetic
NK1
agonist, had lowest effect and senktide, the synthetic NK3 agonist, was far less active than eledoisin, kassinin and
neurokinin A
. Thus, specific
tachykinin
receptors exist in the rat brain that mediate gastric functions: NK3 receptors participate in the control of gastric secretion, while NK2 receptors seem to be involved in the regulation of gastric emptying by activating inhibitory pathways.
...
PMID:Tachykinins: effects on gastric secretion and emptying in rats. 217 57
Contraction of longitudinal muscle strips of the guinea-pig ileum induced by the selective NK3 receptor agonist, succ-[Asp6,MePhe8]SP-(6-11) (senktide), were completely inhibited by tetrodotoxin and partially blocked by atropine. The atropine-resistant contraction was markedly reduced if the smooth muscle
tachykinin
receptors were either desensitized with the selective
NK1
agonist
substance P
methyl ester, or blocked with the
tachykinin
receptor antagonist [D-Pro4,D-Trp7,9,10]SP-(4-11). These results suggest that activation of NK3 receptors on enteric neurones results in acetylcholine and
tachykinin
release.
...
PMID:Evidence for neurokinin-3 receptor-mediated tachykinin release in the guinea-pig ileum. 245 37
We have studied the contractile response and phosphoinositide hydrolysis induced by
substance P
(SP),
neurokinin A
(
NKA
), neurokinin B (NKB), and Alp-Phe-Phe(R)-Gly[ANC-2]-Leu-Met-NH2 (L 363851), a selective NK2-receptor agonist, in guinea pig tracheal smooth muscle. The four tachykinins elicited a concentration-dependent contraction in tracheal smooth muscle devoid of epithelium, with the following order of potency:
NKA
greater than L 363851 greater than NKB greater than SP, (EC50 1.0 x 10(-9) M, 3.2 x 10(-9) M, 7.5 x 10(-9) M and 1.2 x 10(-7) M, respectively), which suggests that NK2 receptors predominate in airway smooth muscle. In the presence of epithelium, the sensitivity of airway smooth muscle to tachykinins was decreased, and the concentration response curves to tachykinins were shifted rightward by 30-fold for SP, 9-fold for
NKA
, and 5-fold for NKB. The concentration response curve to L 363851 was not significantly shifted in the presence of epithelium. This suggests that epithelium may release a relaxant factor in response to tachykinins via an
NK1
receptor. In airway smooth muscle, we found that tachykinins elicited phosphoinositide breakdown with an order of potency similar to that for contractile response (EC50 2.2 x 10(-5) M, 3.6 x 10(-5) M, 4.4 x 10(-5) M, and 5.9 x 10(-5) M). In epithelium, SP alone elicited a significant phosphoinositide breakdown, suggesting that epithelial receptors to tachykinins may be of the
NK1
subtype. Since it is established that phosphoinositide derivatives can elicit mobilization of intracellular calcium, our results suggest that phosphoinositide breakdown is the coupling mechanism for
tachykinin
-induced contraction of airway smooth muscle.
...
PMID:Tachykinin-induced phosphoinositide breakdown in airway smooth muscle and epithelium: relationship to contraction. 245 69
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