NS-398 (CAS: 123653-11-2)
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SKU-Pack Size | Availability | Size | Price | |
EBC51045-1ML | In Stock | 1mL(10mM in DMSO) | €76.70 | |
EBC51045-5MG | In Stock | 5mg | €63.70 | |
EBC51045-10MG | In Stock | 10mg | €89.70 | |
EBC51037-25MG | In Stock | 25mg | €167.70 | |
EBC51045-50MG | In Stock | 50mg | €271.70 |
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Product Information | |||||||||||||||||||||
Synonym(s) | NS 398, NS398 | ||||||||||||||||||||
Chemical Name | N-[2-(cyclohexyloxy)-4-nitrophenyl]-methanesulfonamide | ||||||||||||||||||||
Application | NS-398 is a selective Cox-2 inhibitor neuroprotective agent | ||||||||||||||||||||
CAS Number | 123653-11-2 | ||||||||||||||||||||
Purity | ¡Ý99.0% | ||||||||||||||||||||
Molecular Weight | 314.36 | ||||||||||||||||||||
Molecular Formula | C₁₃H₁₈N₂O₅S | ||||||||||||||||||||
SMILES | CS(=O)(NC1=CC=C([N+]([O-])=O)C=C1OC2CCCCC2)=O | ||||||||||||||||||||
Target & IC50 | COX-1: IC50 = 75 ¦ÌM COX-2: IC50 = 1.77 ¦ÌM |
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Solubility | DMSO: 62 mg/mL (197.23 mM) | ||||||||||||||||||||
Preparing Stock Solutions |
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Shipping | Gel Pack | ||||||||||||||||||||
Storage | Store at -20¡ãC | ||||||||||||||||||||
Research Use | For Research Use Only. Not Intended for Diagnostic Or Therapeutic Use. |
Product Description | |
NS-398 is a small molecule inhibitor of Cox (cyclooxygenase), relatively selective for Cox-2 (IC50 of 3.8 μM) over Cox-1 (IC50 of > 100 μM). The inflammatory response to injury and stimulus is associated with Cox-2 activity, and this activity is thought to be related to neurotoxicity presented in the progression of cerebral ischemia. NS-398 intervenes upon this progression through inhibition of Cox-2, potentially by suppressing the synthesis of Cox-2 reaction products such as prostanoids and superoxide radicals. Additionally, NS-398 is shown to reduce the extent of neuronal damage caused by glutamate excitotoxicity and by N-methyl-D-aspartate injection through blocking the Cox-2 response. Another report assessing Cox-2-mediated neuronal damage associated with methamphetamine further indicates that reactive oxygen species generated by Cox-2 are culprit in this process, rather than prostaglandin expression strongly associated with Cox enzymes and the inflammatory response. |
Specific Protocols | |