Scientists Unveil Structure of Molecular Target of Many Drugs
More than 40 years after beta blockers were first used clinically, scientists can finally get a detailed, three-dimensional look at the drugs’ molecular target—the beta2-adrenergic receptor. This receptor hails from a family of proteins called G protein-coupled receptors (GPCRs) that control critical bodily functions, several of our senses, and the action of about half of today’s pharmaceuticals. Because this is the first known structure of a human GPCR, the work promises not only to speed the discovery of new and improved drugs, but also to broaden our understanding of human health and disease.
To solve the new structure, the researchers overcame daunting scientific obstacles. Many of these difficulties arise because GPCRs are membrane proteins—some of the trickiest molecules to capture in three-dimensional detail because they resist forming crystals, which are needed for structure determination.
Scientists across the country have tried for years to obtain detailed images of GPCR proteins. They’ve succeeded only once before, in 2000, when a research group determined the structure of a visual pigment in cow eyes. Part of the job was easier then, because the pigment protein is abundant. One of the major challenges in the new study was getting enough of the beta2-adrenergic receptor protein to work with.
After trying in
vain to get the protein in its natural form to crystallize, Brian Kobilka and co-workers at
“This is an absolutely remarkable advance,” said Jeremy M. Berg, Ph.D., director of NIGMS, which, in addition to spearheading the PSI, plays a leading role in the membrane protein Roadmap initiative. “Many laboratories around the world are trying to reveal the secrets of these proteins, and this important structure takes the field to a higher level.”
Source: NIH news bulletin
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