>>Signaling Pathways>> Angiogenesis>> PAR1>>PAR-4 Agonist Peptide, amide (AY-NH2)

PAR-4 Agonist Peptide, amide (AY-NH2) (Synonyms: PAR-4-AP; AY-NH2)

Catalog No.GC15817

PAR-4 Agonist Peptide, amide(AY-NH2) (PAR-4-AP; AY-NH2)는 proteinase-activated receptor-4 (PAR-4) agonist로 PAR-1 또는 PAR- 2 및 그의 효과는 PAR-4 길항제에 의해 차단됩니다.

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PAR-4 Agonist Peptide, amide (AY-NH2) Chemical Structure

Cas No.: 352017-71-1

Size 가격 재고 수량
1mg
US$54.00
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Sample solution is provided at 25 µL, 10mM.

Description Protocol Chemical Properties Product Documents Related Products

AY-NH2 is a selective agonist of PAR4 with EC50 value of 11 μM [1].

Protease-activated receptor-4 (PAR4) is a member of PARs and plays an important role in mediating cellular effects of thrombin through acting G-proteins i, 12/13 (Rho and Ras activation) and q (calcium signaling) [2].

AY-NH2 is a potent PAR4 agonist and has a higher (~10 fold) activity than GYPGKF-NH2. Using rat platelet aggregation assay, it was shown that AY-NH2 had highly platelet aggregation ability than GY-NH2 and GF-NH2 [1]. When tested with platelet-rich plasma harvested from wild-type C57BL6 mice, AY-NH2 treatment exhibited highly agonist activity on PAR4 while had no effect on other PARs [3].

In male Wistar rats model of paw oedema, i.pl. injection of AY-NH2 markedly reduced the nociceptive score in response to both noxious and non-noxious mechanical stimuli, thus inhibiting carrageenan-induced mechanical hyperalgesia and allodynia [4].

References:
[1].  Hollenberg, M.D., et al., Proteinase-activated receptor-4: evaluation of tethered ligand-derived peptides as probes for receptor function and as inflammatory agonists in vivo. Br J Pharmacol, 2004. 143(4): p. 443-54.
[2].  Yu, G., et al., Increased expression of protease-activated receptor 4 and Trefoil factor 2 in human colorectal cancer. PLoS One, 2015. 10(4): p. e0122678.
[3].  Faruqi, T.R., et al., Structure-function analysis of protease-activated receptor 4 tethered ligand peptides. Determinants of specificity and utility in assays of receptor function. J Biol Chem, 2000. 275(26): p. 19728-34.
[4].   Asfaha, S., et al., Protease-activated receptor-4: a novel mechanism of inflammatory pain modulation. Br J Pharmacol, 2007. 150(2): p. 176-85.

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