Functional reconstitution of β2-adrenergic receptors utilizing self-assembling Nanodisc technology

Author:

Leitz Andrew J.1,Bayburt Timothy H.1,Barnakov Alexander N.2,Springer Barry A.2,Sligar Stephen G.1

Affiliation:

1. University of Illinois, Urbana, IL

2. Johnson & Johnson Pharmaceutical Research & Development, Exton, PA, USA

Abstract

Integral membrane G protein-coupled receptors (GPCRs) compose the single most prolific class of drug targets, yet significant functional and structural questions remain unanswered for this superfamily. A primary reason for this gap in understanding arises from the difficulty of forming soluble, monodisperse receptor membrane preparations that maintain the trans-membrane signaling activity of the receptor and provide robust biophysical and biochemical assay systems. Here we report a technique for self-assembling functional 2-adrenergic receptor (β2AR) into a nanoscale phospholipid bilayer system (Nanodisc) that is highly soluble in aqueous solution. The approximately 10-nm nanobilayer particles contain β2AR in a native-like phospholipid bilayer domain of approximately 100 phospholipid molecules circumferentially bound by a membrane scaffold protein (MSP). The resulting construct allows for access to the physiologically intracellular and extracellular faces of the receptor and thus allows unrestricted access of antagonists, agonists, and G proteins. These Nanodisc-solubilized GPCRs can be directly purified by normal chromatographic procedures. We define the resultant Nanodisc-embedded monomeric β2AR by antagonist and agonist binding isotherms and demonstrate faithful G protein coupling.

Publisher

Future Science Ltd

Subject

General Biochemistry, Genetics and Molecular Biology,Biotechnology

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