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Novel Molecule Exhibiting Selective Affinity for GABAA Receptor Subtypes.

Sci Rep.. 2017-07;  7(1):6230
Borghese CM1, Herman M2,3, Snell LD4, Lawrence KJ1, Lee HY1, Backos DS5, Vanderlinden LA5, Harris RA1, Roberto M2, Hoffman PL4,6, Tabakoff B.
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PCR Cloning and Subcloning ...The complementary DNAs encoding the GABAA subunits rat α1, β1, β3, γ2 s, δ, and human β2 were provided by Drs Myles H. Akabas, Paul J. Whiting and Richard W. Olsen. Human γ1 cDNA was synthesized de novo, optimized for Xenopus laevis oocyte expression and subcloned in pGEMHE by <b>GenScript</b> (Piscataway, NJ)... Get A Quote

摘要

Aminoquinoline derivatives were evaluated against a panel of receptors/channels/transporters in radioligand binding experiments. One of these derivatives (DCUK-OEt) displayed micromolar affinity for brain γ-aminobutyric acid type A (GABAA) receptors. DCUK-OEt was shown to be a positive allosteric modulator (PAM) of GABA currents with α1β2γ2, α1β3γ2, α5β3γ2 and α1β3δ GABAA receptors, while having no significant PAM effect on αβ receptors or α1β1γ2, α1β2γ1, α4β3γ2 or α4β3δ receptors. DCUK-OEt modulation of α1β2γ2 GABAA receptors was not blocked by flumazenil. The subunit requirements for DCUK-OEt actions distinguished DCUK-OEt from other currently known modulators of GABA function (e... More

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