AI Article Synopsis
- The main challenge in pharmaceutical research is getting integral membrane proteins in a usable form that mimics their natural state, as these proteins are crucial drug targets like receptors and enzymes.
- An example discussed is the 7-transmembrane segment proteins, specifically G-protein-coupled receptors, which are important for drug discovery.
- The article presents a method to self-assemble bacteriorhodopsin with phospholipids, creating a soluble bilayer that incorporates integral membrane proteins, enabling better structural and functional analysis in a lab setting.
Article Abstract
One of the biggest challenges in pharmaceutical research is obtaining integral membrane proteins in a functional, solubilized, and monodisperse state that provides a native-like environment that maintains the spectrum of in vivo activities. Many of these integral membrane proteins are receptors, enzymes, or other macromolecular assemblies that are important drug targets. An example is the general class of proteins composed of seven-transmembrane segments (7-TM) as exemplified by the G-protein-coupled receptors. In this article, we describe a simple system for self-assembling bacteriorhodopsin, as a model protein containing 7-TM helices, with phospholipids to form a nanometer-scale soluble bilayer structure encircled by a 200 amino acid scaffold protein. The result is the single molecule incorporation of an integral membrane protein target into a soluble and monodisperse structure that allows the structural and functional tools of solution biochemistry to be applied.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2366955 | PMC |
| http://dx.doi.org/10.1110/ps.03267503 | DOI Listing |
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