Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.

Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.

The abundance and physiological importance of GABAA receptors in the central nervous system make this neurotransmitter receptor an attractive target for localizing diagnostic and therapeutic biomolecules. GABAA receptors are expressed within the retina and mediate synaptic signaling at multiple stag...

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Main Authors: Sujatha P Koduvayur, Hélène A Gussin, Rajni Parthasarathy, Zengping Hao, Brian K Kay, David R Pepperberg
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3929611?pdf=render
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spelling doaj-2e81072dc8494f7c8850776891cd50292020-11-25T00:43:58ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0192e8796410.1371/journal.pone.0087964Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.Sujatha P KoduvayurHélène A GussinRajni ParthasarathyZengping HaoBrian K KayDavid R PepperbergThe abundance and physiological importance of GABAA receptors in the central nervous system make this neurotransmitter receptor an attractive target for localizing diagnostic and therapeutic biomolecules. GABAA receptors are expressed within the retina and mediate synaptic signaling at multiple stages of the visual process. To generate monoclonal affinity reagents that can specifically recognize GABAA receptor subunits, we screened two bacteriophage M13 libraries, which displayed human scFvs, by affinity selection with synthetic peptides predicted to correspond to extracellular regions of the rat α1 and β2 GABAA subunits. We isolated three anti-β2 and one anti-α1 subunit specific scFvs. Fluorescence polarization measurements revealed all four scFvs to have low micromolar affinities with their cognate peptide targets. The scFvs were capable of detecting fully folded GABAA receptors heterologously expressed by Xenopus laevis oocytes, while preserving ligand-gated channel activity. Moreover, A10, the anti-α1 subunit-specific scFv, was capable of detecting native GABAA receptors in the mouse retina, as observed by immunofluorescence staining. In order to improve their apparent affinity via avidity, we dimerized the A10 scFv by fusing it to the Fc portion of the IgG. The resulting scFv-Fc construct had a Kd of ∼26 nM, which corresponds to an approximately 135-fold improvement in binding, and a lower detection limit in dot blots, compared to the monomeric scFv. These results strongly support the use of peptides as targets for generating affinity reagents to membrane proteins and encourage investigation of molecular conjugates that use scFvs as anchoring components to localize reagents of interest at GABAA receptors of retina and other neural tissues, for studies of receptor activation and subunit structure.http://europepmc.org/articles/PMC3929611?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Sujatha P Koduvayur
Hélène A Gussin
Rajni Parthasarathy
Zengping Hao
Brian K Kay
David R Pepperberg
spellingShingle Sujatha P Koduvayur
Hélène A Gussin
Rajni Parthasarathy
Zengping Hao
Brian K Kay
David R Pepperberg
Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
PLoS ONE
author_facet Sujatha P Koduvayur
Hélène A Gussin
Rajni Parthasarathy
Zengping Hao
Brian K Kay
David R Pepperberg
author_sort Sujatha P Koduvayur
title Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
title_short Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
title_full Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
title_fullStr Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
title_full_unstemmed Generation of recombinant antibodies to rat GABAA receptor subunits by affinity selection on synthetic peptides.
title_sort generation of recombinant antibodies to rat gabaa receptor subunits by affinity selection on synthetic peptides.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description The abundance and physiological importance of GABAA receptors in the central nervous system make this neurotransmitter receptor an attractive target for localizing diagnostic and therapeutic biomolecules. GABAA receptors are expressed within the retina and mediate synaptic signaling at multiple stages of the visual process. To generate monoclonal affinity reagents that can specifically recognize GABAA receptor subunits, we screened two bacteriophage M13 libraries, which displayed human scFvs, by affinity selection with synthetic peptides predicted to correspond to extracellular regions of the rat α1 and β2 GABAA subunits. We isolated three anti-β2 and one anti-α1 subunit specific scFvs. Fluorescence polarization measurements revealed all four scFvs to have low micromolar affinities with their cognate peptide targets. The scFvs were capable of detecting fully folded GABAA receptors heterologously expressed by Xenopus laevis oocytes, while preserving ligand-gated channel activity. Moreover, A10, the anti-α1 subunit-specific scFv, was capable of detecting native GABAA receptors in the mouse retina, as observed by immunofluorescence staining. In order to improve their apparent affinity via avidity, we dimerized the A10 scFv by fusing it to the Fc portion of the IgG. The resulting scFv-Fc construct had a Kd of ∼26 nM, which corresponds to an approximately 135-fold improvement in binding, and a lower detection limit in dot blots, compared to the monomeric scFv. These results strongly support the use of peptides as targets for generating affinity reagents to membrane proteins and encourage investigation of molecular conjugates that use scFvs as anchoring components to localize reagents of interest at GABAA receptors of retina and other neural tissues, for studies of receptor activation and subunit structure.
url http://europepmc.org/articles/PMC3929611?pdf=render
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