Comparison

SR3335

Item no. CS-1044-50mg
Manufacturer ChemScene
Amount 50mg
Category
Type Molecules
Specific against other
ECLASS 10.1 32169090
ECLASS 11.0 32169090
UNSPSC 12000000
Similar products 293753-05-6
Available
Alternative Names
ML 176
CAS
293753-05-6
Purity
>98%
Formula
C13H9F6NO3S2
MWt
405.34
Solubility
DMSO : >= 100 mg/mL (246.71 mM)
Clinical Information
No Development Reported
Pathway
Metabolic Enzyme/Protease
Target
ROR
Biological Activity
SR3335 is a selective RORalpha synthetic ligand, directly binds to RORalpha (Ki 220 nM) but not other RORs, and functions as a selective partial inverse agonist of RORalpha in cell-based assays. IC50 & Target: Ki: 220 nM (RORalpha)[1] In Vitro: SR3335 is a selective RORalpha partial inverse agonist. In a biochemical radioligand binding assay using [3H]25-hydroxycholesterol as a label it is clear that unlabeled SR3335 dose-dependently competes for binding to the RORalpha LBD. The Ki is calculated as 220 nM using the Cheng-Prusoff equation. In a cell-based chimeric receptor Gal4 DNA-binding domain-NR ligand binding domain cotransfection assay, SR3335 significantly inhibits the constitutive transactivation activity of RORalpha (IC50=480 nM)(partial inverse agonist activity), but has no effect on the activity of LXRalpha and RORgamma[1]. In Vivo: Pharmacokinetic studies indicate that SR3335 displays reasonable exposure following an i.p. injection into mice. The ability of SR3335 is assessed to suppress gluconeogenesis using a diet induced obesity (DIO) mouse model where the mice where treated with 15 mg/kg b.i.d., i.p. for 6-days followed by a pyruvate tolerance test. SR3335 treated mice displays lower plasma glucose levels following the pyruvate challenge consistent with suppression of gluconeogenesis. Importantly, mice treated with SR3335 displayed no difference in body weight or food intake after 7-days of treatment with SR3335[1].

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All products are intended for research use only (RUO). Not for human, veterinary or therapeutic use.

Amount: 50mg
Available: In stock
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