Muscle contraction: a mechanism of energy transduction

A mechanism of muscle contraction is presented in which energy from the hydrolysis of MgATP is transferred directly to conformational strain in a flexible segment of the myosin head. That segment is proximal to both the active site and the subfragment 1—subfragment 2 hinge (the portion of the myosin molecule that connects each of its two enzymatically active globular heads to the long thin helical body). This proximity allows configurational changes at the active site, which are an intrinsic part of the enzymatic mechanism, to impose a localized strain, or distortion, near the hinge. The energy, trapped in the protein this way, is subsequently used for mechanical work when other enzymatically-induced conformational changes free the strained segment of the myosin head to unbend. As this happens, the head rotates and the distal end (opposite the hinge) attaches to the actin filament and pulls on it. In this mechanism, actin interacts with myosin in two different ways: (1) at the active site where it activates a step in the hydrolysis of MgATP that frees the head to rotate; (2) at the distal end of myosin, where it forms the grip through which the rotating head pulls on the actin filament. The first interaction allows actin to initiate primary movement of the myosin head; the second directs the force and allows the movement of the head to be used for the sliding motion of the actin and myosin filaments during contraction. In this model, there are also two different energy transfers: one occurs in the transduction process itself when energy from hydrolysis is trapped as conformational distortion in the hinge region; the other occurs, reversibly, when actin and myosin form and then break the distal grip; in this second transfer there is no net energy change in the course of a cycle. A chemical mechanism is suggested to explain actin-activation of hydrolysis at the active site-hinge region.