Researchers Capture Images of a Protein Complex That Keeps Heart Beating

Fast facts:

  • Some genetic mutations linked to sudden cardiac death are known to affect a certain part of sodium channels, the proteins responsible for letting sodium ions into cells
  • Researchers found the effect of these mutations on the interaction between sodium channels and another protein, calmodulin, which regulates the channels’ opening
  • This discovery suggests a starting point for designing drugs to prevent sudden cardiac death

For years, a multidisciplinary team of Johns Hopkins researchers has tracked an elusive creature, a complex of proteins thought to be at fault in some cases of sudden cardiac death. As they report November 5 in the online edition of Nature Communications, they have finally captured images of the complex. Those images reveal the connection between some genetic mutations and electrical abnormalities of the heart and provide a starting point for designing therapies.

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Sudden cardiac death is often caused by conditions that affect electrical signaling in the heart. Genetic studies have linked 2 of these conditions (long QT syndrome and Brugada syndrome) to mutations in the sodium channels that let sodium ions into cells in response to electrical signals. Many of the mutations affect a particular part of the channel that was thought to interact with a protein called calmodulin. This seemed important, because, explains Gordon Tomaselli, MD, the Michel Mirowski, MD Professor of Cardiology at the Johns Hopkins University School of Medicine, “Calmodulin is the most ubiquitous calcium-binding protein in nature, and it regulates the function of sodium channels not only in the heart, but also in the brain and muscle.”

The genetic studies were a hint that many cases of sudden cardiac death might come down to faulty interactions between sodium channels and calmodulin, which in turn would lead to electrical misfires. In that case, perhaps a drug could be designed that would correct the interaction. But finding such a drug would be a shot in the dark unless researchers could figure out what the sodium channel–calmodulin complex looked like, and how the mutations were affecting it.

Tomaselli’s research group teamed with those of L. Mario Amzel, PhD, a professor of biophysics and biophysical chemistry, and Sandra Gabelli, PhD, an assistant professor of medicine and of biophysics and biophysical chemistry, to try to determine the structure of the complex and how changes to it affect muscles’ electrical properties. To learn that, the researchers had to coax bacterial cells to make human versions of sodium channel proteins and calmodulin, purify the protein complexes, and image them with a technique called X-ray crystallography. “We observed that binding to calmodulin changes the state of the sodium channel, leaving it poised to be activated, or opened, by an electrical signal from outside the cell,” Gabelli says.

Previous studies had hinted that poised-for-activation sodium channels tended to be bound not just to calmodulin, but also to a second sodium channel. “As expected, we found that two sodium channels often bind both to each other and to calmodulin,” Amzel says. “We were completely surprised, though, to find that it is the same domain of the two channels that interact with each other.”

The researchers also tested the electrical properties of cells with normal and mutated versions of the sodium channel–calmodulin complex. They found that the latter corresponded with EKG readings of people with long QT and Brugada syndromes.

“Altering calmodulin regulation of sodium channels may be an important and novel therapeutic strategy for the treatment of heart failure, arrhythmias, neurological disorders, such as seizures and autism, and diseases of skeletal muscle,” Tomaselli says.

Other authors on the paper are Agedi Boto, Victoria Halperin Kuhns, Mario A. Bianchet, Federica Farinelli, Srinivas Aripirala, and Jesse Yoder, all of the Johns Hopkins University, and Jean Jakoncic of Brookhaven National Laboratory.

This study was funded by the National Heart, Lung and Blood Institute (grant number HL050411).

The above story is reprinted from materials provided by the John Hopkins Medicine via Newswise.

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