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BioChemicals
Anacetrapib
tcsc0636
Anacetrapib
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100mg
$
1,680.00
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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
Anacetrapib is a potent
CETP
inhibitor, with
IC
50
s of 7.9±2.5 nM and 11.8±1.9 nM for rhCETP and C13S CETP mutant, respectively.
IC50 & Target: IC50: 7.9±2.5 nM (rhCETP), 11.8±1.9 nM (CETP
C13S
)
[1]
In Vitro:
Anacetrapib dose-dependently and significantly decreases the transfer of CE from HDL3 to HDL2 (P<0.001 for concentrations equal to and higher than 0.1 µM). Excess Anacetrapib (25 µM) decreases the amount of [
14
C]Torcetrapib (0.25 µM) binds to immobilized rhCETP by 82% and 60%, respectively. Anacetrapib decreases pre-β-HDL formation by more than 46% (P<0.001) at all concentrations tested (0.1, 1, 3, and 10 µM)
[1]
. A significant reduction of PCSK9 promoter activity by Anacetrapib (ANA) is detected at 3 µM concentration (−22%, p<0.01) and further lowered to 68% of control at 10 µM. Likewise, luciferase activity of B11 cells are decreased by Anacetrapib at 3 µM concentration and reached to a maximal reduction of 38% of control at 10 µM. At 10 µM concentration, Anacetrapib loweres PCSK9 mRNA level to 60% of control and LDLR mRNA level to 67% of control
[2]
.
In Vivo:
Hamsters are given Anacetrapib for 7 days before injection of [
3
H]cholesterol-labeled macrophages (day 0). Treatment with Anacetrapib leads to significant increases in HDL-C levels at day 0. At day 3, [
3
H]cholesterol radioactivity in the HDL fraction is significantly increased from control values for Anacetrapib
[1]
. Anacetrapib (ANA) treatment modestly elevates serum total serum cholesterol levels ~10% (p<0.05) and increases serum LDL-C by 26% (p<0.05) as compared to vehicle control
[2]
. After an intravenous dose of 0.5 mg/kg, the mean values for systemic plasma clearance, steady-state volume of distribution, and terminal half-life are 2.3 mL/min/kg, 1.1 L/kg, and 12 h, respectively. After oral dosing at 5 mg/kg, the bioavailability of Anacetrapib is 38%. Exposures (AUC) increases in a less than dose-proportional manner from 23 μM•h at 5 mg/kg to 362 μM•h at 500 mg/kg. In this dose range, the peak plasma level (C
max
) ranges from 5 to 26 μM and the time to reach peak plasma level (T
max
) ranged from 3 to 4.5 h
[3]
.
Information
CAS No
875446-37-0
Formula
C
30
H
25
F
10
NO
3
Clinical Information
clinicalinformation
Pathway
Metabolic Enzyme/Protease
Target
CETP
Specifications
Purity / Grade
>98%
Solubility
10 mM in DMSO
Smiles
smiles
Misc Information
Alternative Names
MK-0859
Observed Molecular Weight
637.51
related data
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