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BioChemicals
Reparixin (L-lysine salt)
tcsc1380
Reparixin (L-lysine salt)
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AVAILABLE SIZES
5mg
10mg
50mg
$
514.00
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ORDERING INFORMATION
International
TAICLONE BIOTECH CORP.
order@taiclone.com
+886-2-2735-9682
+886-2-2735-9807
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Product Description
Reparixin L-lysine salt is a potent and specific allosteric inhibitor of both CXCL8 receptors
CXCR1/2
, it inhibits weakly
CXCR2
-mediated cell migration (
IC
50
=100 nM), whereas it strongly blocks
CXCR1
-mediated chemotaxis (
IC
50
=1 nM).
IC50 & Target: IC50: 5.6/80 nM (CXCR1
wt
/CXCR1
Ile43Val
, in L1.2 cell)
[1]
In Vitro:
Reparixin is a potent functional inhibitor of CXCL8-induced biological activities on human PMNs with a marked selectivity (around 400-fold) for CXCR1, as shown in specific experiments on CXCR1/L1.2 and CXCR2/L1.2 transfected cells and on human PMNs. The efficacy of Reparixin is significantly lower in L1.2 cells expressing Ile43Val CXCR1 mutant (IC
50
values of 5.6 nM and 80 nM for CXCR1 wt and CXCR1 Ile43Val, respectively)
[1]
. Reparixin is a non-competitive allosteric inhibitor of IL-8 receptors with a 400-fold higher efficacy in inhibiting CXCR1 activity than CXCR2
[2]
.
In Vivo:
The pharmacokinetics and metabolism of Reparixin are investigated in rats and dogs after intravenous administration of [
14
C]-Reparixin L-lysine salt. Plasma protein binding of Reparixin is >99% in the laboratory animals and humans up to 50 µg/mL, but lower at higher concentrations. Although radioactivity is rapidly distributed into rat tissues, V
ss
is low (about 0.15 L/kg) in both rat and dog. Nevertheless, Reparixin is more rapidly eliminated in rats (t
1/2
~0.5 h) than in dogs (t
1/2
~10 h)
[3]
.
Information
CAS No
266359-93-7
Formula
C
20
H
35
N
3
O
5
S
Clinical Information
clinicalinformation
Pathway
GPCR/G Protein
Immunology/Inflammation
Target
CXCR
CXCR
Specifications
Purity / Grade
>98%
Solubility
H2O : ≥ 200 mg/mL (465.58 mM)
Smiles
smiles
Misc Information
Alternative Names
Repertaxin L-lysine salt
Observed Molecular Weight
429.57
related data
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