Selective mGAT2 (BGT-1) GABA Uptake Inhibitors: Design, Synthesis, and Pharmacological Characterization

Stine B. Vogensen,Lars N. Jorgensen,Karsten K. Madsen,Nrupa Borkar,Petrine Wellendorph,Jonas Skovgaard-Petersen,Arne Schousboe,H. Steve White,Povl Krogsgaard-Larsen,Rasmus P. Clausen

Selective mGAT2 (BGT-1) GABA Uptake Inhibitors: Design, Synthesis, and Pharmacological Characterization

2013

Stine B. Vogensen
Lars N. Jorgensen
Karsten K. Madsen
Nrupa Borkar
Petrine Wellendorph
Jonas Skovgaard-Petersen
Arne Schousboe
H. Steve White
Povl Krogsgaard-Larsen
Rasmus P. Clausen

β-Amino acids sharing a lipophilic diaromatic side chain were synthesized and characterized pharmacologically on mouse GABA transporter subtypes mGAT1–4. The parent amino acids were also characterized. Compounds 13a, 13b, and 17b displayed more than 6-fold selectivity for mGAT2 over mGAT1. Compound 17b displayed anticonvulsive properties inferring a role of mGAT2 in epileptic disorders. These results provide new neuropharmacological tools and a strategy for designing subtype selective GABA transport inhibitors.

Keywords:

Selectivity
Side chain
GABA transporter
GABA Uptake Inhibitors
Amino acid
GABA transport
Biochemistry
Stereochemistry
Chemistry
design synthesis
subtype selective

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