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BioChemicals
TRAM-34
tcsc1921
TRAM-34
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AVAILABLE SIZES
10mg
50mg
100mg
$
686.00
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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
TRAM-34 is a highly selective blocker of intermediate-conductance calcium-activated K
+
channel (
IKCa1
) (
K
d
=20 nM).
IC50 & Target: Kd: 20 nM (IKCa1)
[1]
In Vitro:
TRAM-34 selectively blocks the IKCa1 current (K
d
=25 nM), TRAM-34 also blocks IKCa1 currents in human T84 colonic epithelial cells with equivalent potency (K
d
=22 nM). TRAM-34 inhibits the cloned and the native IKCa1 channel in human T lymphocytes with a K
d
of 20-25 nM and is 200- to 1,500-fold selective over other ion channels. The dose-response curve reveals a K
d
of 20±3 nM and a Hill coefficient of 1.2 with 1 μM calcium in the pipette
[1]
. TRAM-34, a specific inhibitor of K
Ca
3.1 channels increased or decreased cell proliferation depending on the concentration. At intermediate concentrations (3-10 µM) TRAM-34 increased cell proliferation, whereas at higher concentrations (20-100 µM) TRAM-34 decreased cell proliferation. The enhancement of cell proliferation caused by TRAM-34 is blocked by the oestrogen receptor antagonists ICI182,780 and tamoxifen. TRAM-34 also increases progesterone receptor mRNA expression, decreased oestrogen receptor-α mRNA expression and reduced the binding of radiolabelled oestrogen to MCF-7 oestrogen receptor, in each case mimicking the effects of 17β-oestradiol
[2]
.
In Vivo:
Mice (n=5) injected intravenously with a single dose of TRAM-34 (0.5 mg/kg; 29 μM) appeared clinically normal during the 7-day study. The body-weight data of the TRAM-34-treated group (day 1:17.8 g; day 7: 27.0 g) are similar to control mice injected with the vehicle (day 1: 17.4 g; day 7: 23.4 g). Collectively, data from these limited toxicity studies suggest that TRAM-34 is not acutely toxic at ≈500-1,000 times the channel-blocking dose
[1]
.Treatment with TRAM-34 results in a significant reduction in hematoxylin & eosin (H&E) defined lesion area with the mean infarct size being reduced from 22.6±3.6% in the controls (n=8) to 11.3±2.8% in rats treated with 10 mg/kg TRAM-34 (n=6, mean±s.e.m., P=0.039) and to 8.1±1.9% in rats treated with 40 mg/kg TRAM-34 (n=8; P=0.004). The treatment also tended to reduce brain shrinkage. However, the results are only statistically significant with 40 mg/kg TRAM-34 (P=0.013), but not for the 10 mg/kg group (P=0.11)
[3]
.
Information
CAS No
289905-88-0
Formula
C
22
H
17
ClN
2
Clinical Information
clinicalinformation
Pathway
Membrane Transporter/Ion Channel
Target
Potassium Channel
Specifications
Purity / Grade
>98%
Solubility
DMSO : ≥ 3.5 mg/mL (10.15 mM)
Smiles
smiles
Misc Information
Observed Molecular Weight
344.84
related data
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