Coupling Between Myosin ATPase Cycle and Creatine Kinase Cycle Facilitates Cardiac Actomyosin Sliding In Vitro : A Clue to Mechanical Dysfunction During Myocardial Ischemia

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Circulation. 1996;93:310-317

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Coupling Between Myosin ATPase Cycle and Creatine Kinase Cycle Facilitates Cardiac Actomyosin Sliding In Vitro

A Clue to Mechanical Dysfunction During Myocardial Ischemia

Masataka Sata, MD; Seiryo Sugiura, MD; Hiroshi Yamashita, MD; Shin-ichi Momomura, MD; Takashi Serizawa, MD

From the Second Department of Internal Medicine, Faculty of Medicine, University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo 113, Japan.

Correspondence to Masataka Sata, MD, Department of Physiology, University of Massachusetts Medical Center, 55 Lake Ave N, Worcester, MA 01655-0127. E-mail mxs125@po.cwru.edu.

Background There is much evidence to support the favorable effectsof the phosphocreatine shuttle on myocardial contraction andrelaxation. However, experiments in which cardiac muscle fiberor myofibril was used have not elucidated its precise mechanism.

Methods and Results Active movements of fluorescently labeledactin filaments on a cardiac myosin layer coimmobilized withcreatine kinase (CK) onto a nitrocellulose-coated glass coverslipwere studied under various concentrations of adenine nucleotides.At a constant phosphocreatine concentration (5 mmol/L, pH 7.1),the relation of sliding velocity to MgATP concentration followedMichaelis-Menten kinetics. The apparent K_m was significantlysmaller in the presence of CK (0.041±0.001 mmol/L) than inthe absence of CK (0.080±0.001 mmol/L), indicating thatcoattached CK facilitated the propelling of actin filamentsby the myosin ATPase. This phenomenon was also seen under acidicconditions (pH 6.7) as well as in the presence of inorganicphosphate (10 mmol/L). At a constant MgATP concentration (1mmol/L), the inhibitory effect of MgADP on the actin-myosininteraction was weaker in the presence of CK than in the absenceof CK. Another ATP-regenerating system, pyruvate kinase andphospho(enol)pyruvate, while maintaining a low ratio of [MgADP]to [MgATP], did not reduce the K_m value (0.156±0.001mmol/L), suggesting that the effect of coattached CK was notachieved only by prevention of MgADP accumulation.

Conclusions Coupling between the ATPase cycle and the CK cyclemay serve not only to maintain the ATP concentration withinthe myofibril but also to provide optimal conditions for cardiacactomyosin interaction. Consideration of this coupling willoffer a clue to elucidating the systolic or diastolic dysfunction duringmyocardial ischemia or reperfusion.

Key Words: creatine kinase • mechanics • ischemia

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