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Query: UNIPROT:P15088 (
mast cell
)
14,925
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Endothelin (
ET-1
) is a 21-amino acid, vasoconstrictive peptide originally isolated from endothelial cells. It is one member of a class of potent, purportedly paracrine substances that act at receptors in multiple target organs. Antagonists to the receptor subtypes, ETA and ETB, have been designed around the hydrophobic carboxy-terminus of
ET-1
. The resulting hexapeptides possess low nanomolar receptor affinity, but face formidable challenges to oral delivery, given their peptidic nature. Hence, it was important to discriminate between analogs, as well as to optimize structural features combining binding potency with stability in intestinal fluids and permeability across biological membranes. PD 142893 (Ac-DDip16-Leu-Asp-Ile-Trp21) and PD 145065 (Ac-DBhg16-Leu-Asp-Ile-Ile-Trp21), as well as the N-methyl-isoleucine20 analogs were studies, where DDip = 3,3diphenylalanine and DBhg = 10,11-dihydro-5H-dibenzo[a,d]cycloheptene glycine. Analyses were conducted with specific HPLC methods. Permeabilities across CACO-2 cell monolayers ranged from 2.0x10(-4) to 6.3x10(-4)cm/min. The results suggested that these compounds can be absorbed in vivo, based on comparison of permeabilities with those obtained with reference compounds. Much greater differences were observed between the analogs when stability half-lives were compared after incubation in rat intestinal perfusate. The parent peptides, PD 142893 and PD 145065, were unstable, with half-lives less than 20 min. N-Methylation of Ile20 resulted in large increases in stability half-lives to greater 500 min. Enzyme inhibition studies demonstrated the involvement of
carboxypeptidase A
in production of the primary metabolite, the des-Trp derivative. Identification of the primary metabolite of the parent peptide was made by differential UV scanning at 214/280 nm and mass spectral analyses.
...
PMID:In vitro assessment of oral delivery for hexapeptide endothelin antagonists. 878 9
We have previously discovered a long-lasting enhancement of synaptic transmission in mammal autonomic ganglia caused by immunological activation of ganglionic mast cells. Subsequent to
mast cell
activation, lipid and peptide mediators are released which may modulate synaptic function. In this study we determined whether some
mast cell
-derived mediators, prostaglandin D2 (PGD2; 1.0 microM), platelet aggregating factor (PAF; 0.3 microM) and U44619 (a thromboxane analogue; 1.0 microM), and also endothelin-1 (
ET-1
; 0.5 microM) induce synaptic potentiation in the guinea pig superior cervical ganglion (SCG), and compared their effects on synaptic transmission with those induced by a sensitizing antigen, ovalbumin (OVA; 10 micrograms/ml). The experiments were carried out on SCGs isolated from adult male guinea pigs (200-250 g) actively sensitized to OVA, maintained in oxygenated Locke solution at 37 degrees C. Synaptic potentiation was measured through alterations of the integral of the post-ganglionic compound action potential (CAP). All agents tested caused long-term (LTP; duration > or = 30 min) or short-term (STP; < 30 min) potentiation of synaptic efficacy, as measured by the increase in the integral of the post-ganglionic CAP. The magnitude of mediator-induced potentiation was never the same as the antigen-induced long-term potentiation (A-LTP). The agent that best mimicked the antigen was PGD2, which induced a 75% increase in CAP integral for LTP (antigen: 94%) and a 34% increase for STP (antigen: 91%). PAF-, U44619-, and
ET-1
-induced increases in CAP integral ranged for LTP from 34 to 47%, and for STP from 0 to 26%. These results suggest that the agents investigated may participate in the induction of A-LTP.
...
PMID:Role of mast cell- and non-mast cell-derived inflammatory mediators in immunologic induction of synaptic plasticity. 936 17
The distribution of endothelin (ET)-containing mast cells was immunohistochemically investigated in the rat lung and gastrointestinal tract using antibodies against Big
ET-1
, Big ET-2, Big ET-3, mature ETs and their receptors of ET-A, and ET-B. In the lung, numerous mature ETs-containing mast cells were present in connective tissue around the bronchus, bronchioles and in the interalveolar septa. The number of Big ET-2-containing mast cells was almost the same as that of Big ET-3-containing mast cells, while Big
ET-1
-positive mast cells were fewer than that of the other isopeptides. In all the regions of the gastrointestinal tract, immunoreactivity for mature ETs was found mainly in mast cells of the lamina propria, the number of Big ET-2 and Big ET-3-containing cells was almost the same similar to that found in the lung, while Big
ET-1
-containing cells were very few. Moreover, mast cells in not only lung but also gastrointestinal tract contain both of ET-A and ET-B receptors. Electron-microscopically, ET-immunoreaction products were mainly precipitated in the
mast cell
granules. Hence, we presume that ETs are synthesized in and secreted from mast cells in the rat lung and gastrointestinal tract; they act in an autocrine/paracrine fashion; and their main isopeptides are ET-2 and ET-3.
...
PMID:[Immunocytochemical studies on the endothelin peptides and their receptors in mast cells of the rat lung and gastrointestinal tract]. 977 20
The present study examined the roles of endothelin-converting enzyme (ECE), neutral endopeptidase (NEP) and mast cell chymase as processors of the endothelin (ET) analogues
ET-1
(1-21),
ET-1
(1-31) and big
ET-1
in the trachea of allergic mice. Male CBA/CaH mice were sensitized with ovalbumin (10 microg) delivered intraperitoneal on days 1 and 14, and exposed to aerosolized ovalbumin on days 14, 25, 26 and 27 (OVA mice). Mice were killed and the trachea excised for histological analysis and contraction studies on day 28. Tracheae from OVA mice had 40% more mast cells than vehicle-sensitized mice (sham mice). Ovalbumin (10 microg/ml) induced transient contractions (15+/-3% of the C(max)) in tracheae from OVA mice. The ECE inhibitor CGS35066 (10 microM) inhibited contractions induced by big
ET-1
(4.8-fold rightward shift of dose-response curve; P<0.05), but not those induced by either
ET-1
(1-21) or
ET-1
(1-31). The chymase inhibitors chymostatin (10 microM) and Bowman-Birk inhibitor (10 microM) had no effect on contractions induced by any of the ET analogues used. The NEP inhibitor CGS24592 (10 microM) inhibited contractions induced by
ET-1
(1-31) (6.2-fold rightward shift; P<0.05) but not
ET-1
(1-21) or big
ET-1
. These data suggest that big
ET-1
is processed predominantly by a CGS35066-sensitive ECE within allergic airways rather than by
mast cell
-derived proteases such as chymase. If endogenous
ET-1
(1-31) is formed within allergic airways, it is likely to undergo further conversion by NEP to more active products.
...
PMID:Role of endothelin-converting enzyme, chymase and neutral endopeptidase in the processing of big ET-1, ET-1(1-21) and ET-1(1-31) in the trachea of allergic mice. 1219 21
Endothelin (ET)-1(1-31) is a novel vasoconstrictor peptide produced by human mast cell chymase, which selectively cleaves big
ET-1
at the Try(31)-Gly(32) bond. We investigated the localization of
ET-1
(1-31) in various hamster tissues by immunohistochemistry and compared it to the distribution of
ET-1
(1-21). We found that the localization and amount of
ET-1
(1-31) were different from those of
ET-1
(1-21) in each tissue.
ET-1
(1-31)-like immunoreactivities (IR) in the heart, lung, and adrenal gland were observed in the same areas as
ET-1
(1-21) but were significantly weaker, suggesting that
ET-1
(1-31) might play a role only in
mast cell
/chymase-related pathological conditions in these tissues. In the liver,
ET-1
(1-31)-like IR was strongly detected in Kupffer cells where
ET-1
(1-21)-like IR was seen more weakly. In the kidney,
ET-1
(1-31)-like IR was slightly higher than
ET-1
(1-21). These results suggest that
ET-1
(1-31) might have physiological roles distinct from those of
ET-1
(1-21) in some hamster tissues.
...
PMID:Localization of the 31-amino-acid endothelin-1 in hamster tissue. 1470 74
The objective of this study was to determine whether elevated circulating levels of endothelin (ET)-1 are capable of mediating left ventricular (LV)
mast cell
degranulation and thereby induce matrix metalloproteinase (MMP) activation. After the administration of 20 pg/ml
ET-1
to blood-perfused isolated rat hearts, LV tissue was analyzed for signs of
mast cell
degranulation and MMP activation. Relative to control,
ET-1
produced extensive
mast cell
degranulation as well as a significant increase in myocardial water content (78.8 +/- 1.5% vs. 74.2 +/- 2.2%, P <0.01), a marked 107% increase in MMP-2 activity (P <0.05), and a substantial decrease in collagen volume fraction (0.69 +/- 0.09% vs. 0.99 +/- 0.04%, P <0.001). Although the myocardial edema would be expected to increase ventricular stiffness, compliance was not altered, and moderate ventricular dilatation was observed (end-diastolic volume at end-diastolic pressure of 0 mmHg of 330.2 +/- 22.1 vs. 298.9 +/- 17.4 microl in
ET-1
treated vs. control, respectively, P=0.07). Additionally, pretreatment with the
mast cell
stabilizer nedocromil prevented
ET-1
-induced changes in MMP-2 activity, myocardial water content, collagen volume fraction, and end-diastolic volume. These findings demonstrate that
ET-1
is a potent cardiac
mast cell
secretogogue and further indicate that
ET-1
-mediated
mast cell
degranulation is a potential mechanism responsible for myocardial remodeling.
...
PMID:Endothelin-1 mediates cardiac mast cell degranulation, matrix metalloproteinase activation, and myocardial remodeling in rats. 1523 95
Soon after its identification as a powerful vasoconstrictor peptide, endothelin (
ET-1
) was implicated as a detrimental agent involved in determining the outcome of myocardial ischaemia and reperfusion. Early experimental studies demonstrated that ET(A) selective and mixed ET(A)/ET(B) receptor antagonists can reduce infarct size and prevent ischaemia-induced ventricular arrhythmias in models of ischaemia/reperfusion, implying that
ET-1
acts through the ET(A) receptor to contribute to injury and arrhythmogenesis. However, as our understanding of the physiology of
ET-1
has expanded, the role of
ET-1
in the ischaemic heart appears ever more complex. Recent evidence suggests that
ET-1
exerts actions on the heart that are not only detrimental (vasoconstriction, inhibition of NO production, activation of inflammatory cells), but which may also contribute to tissue repair, such as inhibition of cardiomyocyte apoptosis. In addition,
ET-1
-induced
mast cell
degranulation has been linked to a homeostatic mechanism that controls endogenous
ET-1
levels, which may have important implications for the ischaemic heart. Furthermore the mechanism by which
ET-1
promotes arrhythmogenesis remains controversial. Some studies imply a direct electrophysiological effect of
ET-1
, via ET(A) receptors, to increase monophasic action potential duration (MAPD) and induce early after-depolarisations (EADs), while other studies support the view that coronary constriction resulting in ischaemia is the basis for the generation of arrhythmias. Moreover,
ET-1
can induce cardioprotection (precondition) against infarct size and ventricular arrhythmias, through as yet incompletely understood mechanisms. To enable us to identify the most appropriate means of targeting this system in a therapeutically meaningful way we need to continue to explore the physiology of
ET-1
, both in the normal and the ischaemic heart.
...
PMID:Endothelin and the ischaemic heart. 1624 76
Endothelin (ET)-1 evokes a burning pruritus sensation when injected intradermally in humans and nocifensive behavior when injected into the hind paw of rodents. Because pain and pruritus are clearly distinct nociceptive sensory modalities in humans, the current study evaluates the potential of
ET-1
to elicit scratching behavior in mice. Mice received an intradermal injection of 1-30 pmol
ET-1
; 10 microg of the
mast cell
degranulator compound, 48/80; 100 nmol histamine; or vehicle into the scruff, and the number of scratching bouts displayed during the first 40 mins was recorded.
ET-1
caused dose-dependent scratching bouts, which, like the responses to histamine and compound 48/80, occurred mainly during the first 5 to 10 mins of injection, but fewer episodes were also seen up to 35 mins. The effect of
ET-1
was maximal at 10 pmol (total 40 +/- 7 bouts), a value similar to that caused by histamine (52 +/- 5 bouts) and compound 48/80 (53 +/- 6 bouts). The selective ET(B) receptor agonist, IRL-1620 (10 pmol), was not pruritic per se, and actually inhibited responses to histamine and
ET-1
. Pruritus induced by
ET-1
was inhibited by the ET(A) receptor antagonists, 10 nmol BQ-123 (co-injected; net inhibition, 87%) and 10 mg/kg atrasentan (intraperitoneal administration; net inhibition, 83%), or the ET(B) receptor antagonist, 20 mg/kg A-192621 (intraperitoneal administration; net inhibition, 64%), but the response was augmented by co-injection of the ET(B) receptor antagonist, 3 nmol BQ-788 (net potentiation, 234%). Responses to compound 48/80 or responsiveness of vehicle-treated mice were unaffected by these antagonists. Thus,
ET-1
displays potent pruritic actions in the mouse mediated to a substantial extent via local ET(A) receptors. The findings with IRL-1620 and BQ-788 suggest that local ET(B) receptors exert an antipruritic role, but, for reasons still unknown, the results obtained using systemic A-192621 injection are at variance with this view.
...
PMID:Endothelin-1 causes pruritus in mice. 1674 Oct 66
Endothelin (
ET-1
) has been shown to crucially contribute to UV-induced skin responses such as tanning. To test whether
ET-1
is also involved in early cutaneous reactions to UV, we assessed
ET-1
skin levels in UV-irradiated mice. In correlation with the levels of UV-induced skin inflammation,
ET-1
concentrations increased substantially and continually. Moreover, blocking of
ET-1
receptors (ETA) resulted in significantly decreased cutaneous inflammation following UV irradiation. When we assessed skin responses to
ET-1
injections, we observed prominent
mast cell
degranulation and
mast cell
-dependent inflammation. Since mast cells also critically contributed to UV-induced inflammation, we determined the
ET-1
-dependent inflammatory response to UV in the absence and presence of these cells. Interestingly, ETA blockade did not decrease UV-induced inflammation in
mast cell
-deficient mice, unless these mice had been adoptively transferred with mast cells before irradiation. This indicates that skin inflammation due to UV irradiation is caused in part by
ET-1
acting on skin mast cells.
...
PMID:Inflammatory murine skin responses to UV-B light are partially dependent on endothelin-1 and mast cells. 1693 58
Radiation-induced heart disease is a severe side effect of thoracic radiotherapy. Studies suggest that mast cells play a protective role in radiation-induced heart disease and that the endothelin (ET) system mediates protective effects of mast cells in other disorders. This study examined whether mast cells modulate the cardiac ET system and examined the effects of ET receptor inhibition in a rat model of radiation-induced heart disease. Mast cell-deficient (Ws/Ws),
mast cell
-competent (+/+) and Sprague-Dawley rats received 18 Gy irradiation to the heart. Left ventricular mRNA of
ET1
and its receptors (ETA and ETB) was measured in Ws/Ws and +/+ rats at 1 week and 3 months. Sprague-Dawley rats were treated with the ETA/ETB antagonist bosentan, and at 6 months cardiac changes were assessed using the Langendorff perfused rat heart preparation, immunohistochemistry and real-time PCR. Ws/Ws and +/+ rat hearts did not differ in baseline mRNA. In contrast, +/+ rats hearts exhibited up-regulation of
ET1
after irradiation, whereas Ws/Ws rats hearts did not, suggesting the possibility of interactions between mast cells and the cardiac ET system. Bosentan induced reductions in left ventricular systolic pressure, developed pressure and +dP/dtmax but did not affect fibrosis. Because of the known opposing effects of ETA and ETB, studies with selective antagonists may clarify the role of each receptor.
...
PMID:Influence of endothelin 1 receptor inhibition on functional, structural and molecular changes in the rat heart after irradiation. 1876 54
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