ONO 8130

Modify Date: 2024-07-27 18:06:11

ONO 8130 Structure
ONO 8130 structure
Common Name ONO 8130
CAS Number 459841-96-4 Molecular Weight 500.63
Density N/A Boiling Point N/A
Molecular Formula C25H28N2O5S2 Melting Point N/A
MSDS N/A Flash Point N/A

 Use of ONO 8130


ONO-8130 is an orally active and selective prostanoid EP1 receptor antagonist. ONO-8130 blocks phosphorylation of ERK in the L6 spinal cord. ONO-8130 relieves bladder pain in mice with cyclophosphamide-induced cystitis. ONO-8130 can be used for interstitial cystitis research[1].

 Names

Name 4-[6-[N-isobutyl-N-(4-methyl-2-thiazolylsulfonyl)amino]indan-5-yloxymethyl]benzoic acid

 ONO 8130 Biological Activity

Description ONO-8130 is an orally active and selective prostanoid EP1 receptor antagonist. ONO-8130 blocks phosphorylation of ERK in the L6 spinal cord. ONO-8130 relieves bladder pain in mice with cyclophosphamide-induced cystitis. ONO-8130 can be used for interstitial cystitis research[1].
Related Catalog
Target

EP1 Receptor

In Vivo ONO-8130 (0.3-30 mg/kg; Oral preadministration, once) strongly prevents both the bladder pain-like behavior and referred hyperalgesia in a dose-dependent manner[1]. ONO-8130 (30 mg/kg; Orally, once) reverses the established cystitis-related bladder pain[1]. ONO-8130 (30 mg/kg; Orally, once) strongly inhibits phosphorylation of ERK in MDH, DCM, and SPN of the L6 spinal cord caused by intravesical administration of PGE2[1]. Animal Model: Female ddY mice (18-22 g, 4-5 weeks old)[1] Dosage: 0.3, 3, 10, and 30 mg/kg Administration: Orally, once Result: Strongly prevented both the bladder pain-like behavior and referred hyperalgesia in a dose-dependent manner, but had slight effect on the increased bladder weight and vascular permeability. Animal Model: Female ddY mice (18-22 g, 4-5 weeks old, established bladder pain caused by IP cyclophosphamide)[1] Dosage: 10, 30 mg/kg Administration: Orally, once (administered 2.75 hours after i.p. cyclophosphamide) Result: Markedly attenuated the bladder pain-like nociceptive behavior and referred hyperalgesia in the acute phase (3.5-4 h after cyclophosphamide). Animal Model: Female ddY mice (18-22 g, 4-5 weeks old, established bladder pain caused by IP cyclophosphamide)[1] Dosage: 30 mg/kg Administration: Orally, once (administered 4.75 hours after i.p. cyclophosphamide) Result: Significantly suppressed the bladder pain-like nociceptive behavior and tended to reduce the referred hyperalgesia in the persistent phase, 5.5-6 hours after cyclophosphamide. Animal Model: Female ddY mice (18-22 g, 4-5 weeks old, intravesical administration of PGE2 at 5 nmol/mouse)[1] Dosage: 30 mg/kg Administration: Orally, once Result: Strongly inhibited phosphorylation of ERK in MDH, DCM, and SPN of the L6 spinal cord caused by intravesical administration of PGE2 at 5 nmol/mouse, exerted complete blockade in DCM, while its inhibitory effects in MDH and SPN were partial.
References

[1]. Miki T, et al. ONO-8130, a selective prostanoid EP1 receptor antagonist, relieves bladder pain in mice with cyclophosphamide-induced cystitis. Pain. 2011 Jun;152(6):1373-1381.

 Chemical & Physical Properties

Molecular Formula C25H28N2O5S2
Molecular Weight 500.63
Exact Mass 500.14400
PSA 133.42000
LogP 6.14950
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