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H-SER-LEU-ILE-GLY-LYS-VAL-NH2

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Products Intro: Product Name:Protease-Activated Receptor-2, amide
CAS:190383-13-2
Purity:98% Package:1KG;10KG;50KG
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Products Intro: Product Name:H-SER-LEU-ILE-GLY-LYS-VAL-NH2
CAS:190383-13-2
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Products Intro: Product Name:Protease-Activated Receptor-2, amide
CAS:190383-13-2
Purity:98% Package:25mg Remarks:BOC Sciences also provides custom synthesis services for Protease-Activated Receptor-2, amide.
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Products Intro: Product Name:Protease-Activated Receptor-2, PAR-2 Agonist, amide
CAS:190383-13-2
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Products Intro: Product Name:H-SER-LEU-ILE-GLY-LYS-VAL-NH2
CAS: 190383-13-2
Purity:99% Package:1KG;7USD

H-SER-LEU-ILE-GLY-LYS-VAL-NH2 manufacturers

H-SER-LEU-ILE-GLY-LYS-VAL-NH2 Basic information
Product Name:H-SER-LEU-ILE-GLY-LYS-VAL-NH2
Synonyms:PROTEASE-ACTIVATED RECEPTOR-2 AGONIST, AMIDE;PROTEINASE ACTIVATED RECEPTOR 2 (1-6) AMIDE (HUMAN);PROTEINASE ACTIVATED RECEPTOR 2 AGONIST PEPTIDE SLIGKV AMIDE, HUMAN;SER-LEU-ILE-GLY-LYS-VAL-AMIDE;SER-LEU-ILE-GLY-LYS-VAL-NH2;SLIGKVAMIDE;SLIGKV-NH2;PAR-2 AGONIST PEPTIDE (SLIGKV) AMIDE, HUMAN
CAS:190383-13-2
MF:C28H54N8O7
MW:614.78
EINECS:
Product Categories:peptide;Immune Cell Signaling and Blood;Immune System Regulation;Immunomodulators and Antibiotics
Mol File:190383-13-2.mol
H-SER-LEU-ILE-GLY-LYS-VAL-NH2 Structure
H-SER-LEU-ILE-GLY-LYS-VAL-NH2 Chemical Properties
Boiling point 1030.3±65.0 °C(Predicted)
density 1.161±0.06 g/cm3(Predicted)
storage temp. -20°C
solubility ≥13.48 mg/mL in EtOH with gentle warming and ultrasonic; ≥62.9 mg/mL in DMSO; ≥66.2 mg/mL in H2O
form solid
pka12.04±0.10(Predicted)
Water Solubility Soluble to 1 mg/ml in water
SequenceH-Ser-Leu-Ile-Gly-Lys-Val-NH2
Safety Information
Safety Statements 22-24/25
WGK Germany 3
MSDS Information
ProviderLanguage
SigmaAldrich English
H-SER-LEU-ILE-GLY-LYS-VAL-NH2 Usage And Synthesis
UsesSLIGKV-NH2 is a PAR2 agonist.
DefinitionChEBI: Ser-Leu-Ile-Gly-Lys-Val-Amide is an oligopeptide.
Biological Activitysligkv-nh2 serves as a protease-activated receptor 2 (par2) agonist. pars are a group of g-protein-coupled receptors existing in several cell types. up to date, four par members including par1 to 4 have been identified, cloned and designated. par2 is expressed in the respiratory and gastrointestinal tracts. it is suggested that the activation of par2 is closely correlated with inflammatory evens in various cells and tissues. par2 has also been identified to induce protease activation and therefore result in systemic hypotension. [1]
Biochem/physiol ActionsProteinase-activated receptor (PAR-2) is a member of proteolytically cleaved receptors. It is activated by a synthetic peptide (SLIGKV), that is exposed after trypsin cleavage of the amino terminus. PAR-2 stimulates an increase in cytosolic Ca2+ ion concentration.
in vitroit was reported that sligkv-nh2 (the par2 activating peptide), by inducing express of par2, could slightly enhanced mucin secretion by human bronchial epithelial cells in vitro. according to this study, compared to cells treated with a control peptide with reversed amino acid sequence, exposure of cells to sligkv-nh2 for 30 mins resulted in a weak but statistically significant increase in mucin secretion at concentrations of 100 and 1000m. in addition, sligkv-nh2 was demonstrated to accelerate cell cycle progression and stimulate the growth of hepg2 cells. [1, 2]
in vivothe ability of par2 agonists to induce contractile responses was investigated in vivo. it was found that mouse par2 activating (sligrl-nh2) and human par2 activating (sligkv-nh2) peptides triggered a concentration-dependent contractile response in guinea-pig gallbladder. [3]
IC 50a protease-activated receptor 2 (par2) agonist with an ic50 of 10.4 m.
storageStore at -20°C
references[1] lin kw, park j, crews al, li yh, adler kb. protease-activated receptor-2 (par-2) is a weak enhancer of mucin secretion by human bronchial epithelial cells in vitro. int j biochem cell b. 2008. 40: 137988.
[2]xie l, zheng y, li x, zhao jy, chen xy, chen l, zhou j, hai o and li f. enhanced proliferation of human hepatoma cells by par-2 agonists via the erk/ap-1 pathway. oncol rep. 2012.28: 1665-72.
[3] tognetto m, trevisani m, maggiore b, navarra g, turini a, guerrini r, bunnett nw, geppetti p and harrison s. evidence that par-1 and par-2 mediate prostanoid-dependent contraction in isolated guinea-pig gallbladder. br.j.pharmacol. 2000.131: 689-94.
[4] robin j, kharbanda r, mclean p, campbell r, vallance p. protease-activated receptor 2–mediated vasodilatation in humans in vivo, role of nitric oxide and prostanoids. circulation. 2003;107:954-959.
H-SER-LEU-ILE-GLY-LYS-VAL-NH2 Preparation Products And Raw materials
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H-SER-LEU-ILE-GLY-LYS-VAL-NH2