Molecular mechanism of allosteric modulation at GPCRs: insight from a binding kinetics study at the human A1 adenosine receptor期刊界 All Journals 搜尽天下杂志传播学术成果专业期刊搜索期刊信息化学术搜索

Molecular mechanism of allosteric modulation at GPCRs: insight from a binding kinetics study at the human A1 adenosine receptor

Authors:

Dong Guo Suzanne N Venhorst Arnault Massink Jacobus P D van Veldhoven Georges Vauquelin Adriaan P IJzerman Laura H Heitman

Affiliation:

1.Division of Medicinal Chemistry, Leiden Academic Centre for Drug Research (LACDR), Leiden University, Leiden, The Netherlands;2.Institute for Molecular Biology and Biotechnology, Free University of Brussels (VUB), Brussel, Belgium

Abstract:

Background and Purpose

Many GPCRs can be allosterically modulated by small-molecule ligands. This modulation is best understood in terms of the kinetics of the ligand–receptor interaction. However, many current kinetic assays require at least the (radio)labelling of the orthosteric ligand, which is impractical for studying a range of ligands. Here, we describe the application of a so-called competition association assay at the adenosine A₁ receptor for this purpose.

Experimental Approach

We used a competition association assay to examine the binding kinetics of several unlabelled orthosteric agonists of the A₁ receptor in the absence or presence of two allosteric modulators. We also tested three bitopic ligands, in which an orthosteric and an allosteric pharmacophore were covalently linked with different spacer lengths. The relevance of the competition association assay for the binding kinetics of the bitopic ligands was also explored by analysing simulated data.

Key Results

The binding kinetics of an unlabelled orthosteric ligand were affected by the addition of an allosteric modulator and such effects were probe- and concentration-dependent. Covalently linking the orthosteric and allosteric pharmacophores into one bitopic molecule had a substantial effect on the overall on- or off-rate.

Conclusion and Implications

The competition association assay is a useful tool for exploring the allosteric modulation of the human adenosine A₁ receptor. This assay may have general applicability to study allosteric modulation at other GPCRs as well.Table of Links

TARGETS	LIGANDS
Adenosine A1 receptor	CCPA	DPCPX
	CPA	NECA

Open in a separate windowThis Table lists key protein targets and ligands in this article which are hyperlinked to corresponding entries in http://www.guidetopharmacology.org, the common portal for data from the IUPHAR/BPS Guide to PHARMACOLOGY (Pawson et al., ) and are permanently archived in the Concise Guide to PHARMACOLOGY 2013/14 (Alexander et al., ).

Keywords:

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