An international team has shown how this cardiac protein interacts with actin, one of the two filament –forming muscle proteins (the other is myosin) that slide past each other to create the rhythmic contraction and relaxation that causes the heart to beat.

"Understanding the structure of this heart protein – called cardiac myosin-binding protein C – and how it attaches to actin, gives us an insight into how it actually works to modulate heart contractions.

"There's a lot of interest in cardiac myosin-binding protein C, because of its influence on fine-tuning heart muscle contractions and its links to familial hypertrophic cardiomyopathy – an inherited cardiac disorder that affects one in 500 adolescents and young adults.

"Young people with familial hypertrophic cardiomyopathy have a gradual thickening of the ventricle walls of their hearts and a correlated increase in the risk of heart failure," said lead researcher Prof Jill Trewhella of the University of Sydney.

However, the precise molecular mechanisms by which cardiac myosin-binding protein C influences actin and myosin interactions have not been fully understood.

Cardiac myosin-binding protein C, known as an "accessory protein" in the muscle cells that keep our hearts beating, is a long molecule made up of eleven segments, called domains, arranged like beads on a string.

Using neutron scattering to examine the structure of cardiac myosin-binding protein C when bound to actin, Prof Trewhella and colleagues at California University found the specific domains of the protein that bind to and stabilise actin filaments.

"It turns out there are two domains of cardiac myosin-binding protein C that bind to actin – the C0 and C1 domains that are at one end of the molecule. Domains at the opposite end are attached to myosin. This is a real first – it's the first direct structural evidence that shows how cardiac myosin-binding protein C stabilises actin filaments.

"We've not only found the particular domains of the protein that bind to actin, but where they bind and how they are positioned to modulate the interactions between actin and myosin and hence the contractile cycle," said Prof Trewhella.