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Aminooxyacetic acid hemihydrochloride

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Catalog No. T5880Cas No. 2921-14-4
Alias Carboxymethoxylamine Hemihydrochloride

Aminooxyacetic acid hemihydrochloride (Carboxymethoxylamine Hemihydrochloride) is a malate-aspartate shuttle (MAS) inhibitor which also inhibits the GABA degradating enzyme GABA-T.

Aminooxyacetic acid hemihydrochloride

Aminooxyacetic acid hemihydrochloride

🥰Excellent
Purity: 98.03%
Catalog No. T5880Alias Carboxymethoxylamine HemihydrochlorideCas No. 2921-14-4
Aminooxyacetic acid hemihydrochloride (Carboxymethoxylamine Hemihydrochloride) is a malate-aspartate shuttle (MAS) inhibitor which also inhibits the GABA degradating enzyme GABA-T.
Pack SizePriceAvailabilityQuantity
500 mg$41In Stock
1 g$68In Stock
1 mL x 10 mM (in DMSO)$45In Stock
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Purity:98.03%
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Product Introduction

Bioactivity
Description
Aminooxyacetic acid hemihydrochloride (Carboxymethoxylamine Hemihydrochloride) is a malate-aspartate shuttle (MAS) inhibitor which also inhibits the GABA degradating enzyme GABA-T.
In vivo
At various intervals after aminooxyacetic acid(AOAA) the rats were either injected with one of the convulsive drugs or sacrificed for analysis of the GABA concentration.?AOAA caused a rapid initial (0-30 min) and a later slower increase of GABA in cerebellum and whole brain.?In the synaptosomal fraction the GABA accumulation was delayed and less pronounced when compared to the whole brain.?The bicuculline induced convulsions were markedly potentiated during the first hour but completely blocked from 2-6 h after AOAA.?Picrotoxin showed a somewhat different pattern to bicuculline in the interactions with AOAA.?The initial strong potentiation was not observed but the later phase of protection was present.?In the interactions with 3-MPA, the effect of AOAA was always protective.?The time to onset of convulsions was gradually increased during the first 30 min after AOAA.?This protective effect remained practically unchanged up to 6 h after AOAA.?However, once started, the convulsions were generally of the same duration and intensity.?The results can be interpreted as GABA accumulating after AOAA stimulates GABA receptors to a degree more or less proportional to the whole brain GABA concentration and further that GABA synthetized in neurons is liberated, stimulates inhibitory bicuculline sensitive (predominant) and excitatory bicuculline insensitive receptors and is captured to a large extent by non-neuronal cells[1].
AliasCarboxymethoxylamine Hemihydrochloride
Chemical Properties
Molecular Weight109.3
FormulaC2H5NO3·0.5HCl
Cas No.2921-14-4
SmilesCl.NOCC(O)=O.NOCC(O)=O
Relative Density.1.7848 g/cm3 (Estimated)
Storage & Solubility Information
StoragePowder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
Solubility Information
DMSO: 45 mg/mL (411.71 mM)
Solution Preparation Table
DMSO
1mg5mg10mg50mg
1 mM9.1491 mL45.7457 mL91.4913 mL457.4565 mL
5 mM1.8298 mL9.1491 mL18.2983 mL91.4913 mL
10 mM0.9149 mL4.5746 mL9.1491 mL45.7457 mL
20 mM0.4575 mL2.2873 mL4.5746 mL22.8728 mL
50 mM0.1830 mL0.9149 mL1.8298 mL9.1491 mL
100 mM0.0915 mL0.4575 mL0.9149 mL4.5746 mL

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