Summary
We have explored a model of crossbridge kinetics that explains many of the effects on steady-state muscle contraction of ligands that bind to the nucleotide site on myosin. The mathematical model follows the basic framework for crossbridge function first established by A. F. Huxley. In the model, detached crossbridges initially bind in a weakly Attached, A.M.D.Pi state (A, actin; M, myosin; D, ADP; Pi, orthophosphate) at the beginning of the region of positive force production. Pi release then results in transition to a strongly-bound A.M.D state, as has been suggested by other investigators from both biochemical and mechanical data. Mg2+ ADP release and subsequent crossbridge detachment due to Mg2+ ATP binding to the A.M state occur at the end of the region of positive force production. Work in a number of laboratories has now defined the effects on steady-state contraction of variations in the concentrations of Mg2+ ATP, Mg2+ ADP and Pi. These data provide valuable constraints that can be used to further refine current models. The maximum velocity of shortening (V max) and ATPase activity of muscle fibres exhibit classical saturation behaviour with respect to Mg2+ ATP concentration, with Mg2+ ADP acting as a competitive inhibitor. The model can reproduce this behaviour. The model also explains the observations that increasing [Mg2+ ATP] decreases isometric tension and increasing [Mg2+ ADP] increases tension. As the concentration of Pi increases, model predictions suggest that tension should decrease approximately as log[Pi], that ATPase activity should decrease less than tension and thatV max should be almost unchanged, as has been found experimentally. The model also demonstrates that the connection between the parameters of contraction and the free energy of hydrolysis of Mg2+ ATP can be complex.
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References
Abbott, R. H. &Mannherz, H. G. (1970) Activation by Mg2+ADP and the correlation between tensions and ATPase activity in insect fibrillar muscle.Pflügers Arch. ges. Physiol. 321, 223–32.
Alberty, R. A. (1968) Effect of pH and metal ion concentration on the equilibrium hydrolysis of adenosine triphosphate to adenosine diphosphate.J. biol. Chem. 243, 1337–43.
Altringham, J. D. &Johnston, I. A. (1985) Effects of phosphate on the contractile properties of fast and slow muscle fibres from an Antarctic fish.J. Physiol. Lond. 468, 491–500.
Bowater, R. &Sleep, J. (1988) Demembrated muscle fibres catalyze a more rapid exchange between phosphate and adenosine triphosphate than actomyosin subfragment 1.Biochemistry 27, 5314–23.
Brenner, B., Chalovich, J. M., Greene, L. E., Eisenberg, E. &Schoenberg, M. (1986) Stiffness of skinned rabbit psoas fibres in MgATP and MgPPi solution.Biophys. J. 50, 685–91.
Brokaw, C. J. (1976) Computer simulation of flagellar movement.Biophys. J. 16, 1029–41.
Chase, P. B. &Kushmerick, M. J. (1988) Effects of pH on contraction of rabbit fast and slow skeletal muscle fibres.Biophys. J. 53, 935–46.
Cooke, R. (1986) The mechanism of muscle contraction.CRC Crit. Rev. Biochem. 21, 53–118.
Cooke, R. &Bialek, W. (1979) Contraction of glycerinated muscle fibers as a function of MgATP concentration.Biophys. J. 28, 241–58.
Cooke, R. &Pate, E. (1985) The effects of ADP and phosphate on the contraction of muscle fibres.Biophys. J. 48, 789–98.
Cooke, R., Franks, K., Lucianni, G. &Pate, E. (1988) The inhibition of rabbit skeletal muscle contraction by hydrogen ions and phosphate.J. Physiol., Lond. 395, 77–97.
Dantzig, J. A., Laktis, J. W., Homsher, E. &Goldman, Y. (1987) Mechanical transients initiated by photolysis of caged Pi during active skeletal muscle contraction.Biophys. J. 51, 3a.
Dawson, M. J., Gadian, D. G. &Wilkie, D. R. (1978) Muscular fatigue investigated by phosphorus nuclear magnetic resonance.Nature 274, 861–6.
Dawson, M. J., Gadian, D. G. &Wilkie, D. R. (1980) Mechanical relaxation rate and metabolism studied in fatiguing muscle by phosphorus nuclear magnetic resonance.J. Physiol., Lond. 299, 465–84.
Eisenberg, E. &Greene, L. (1980) The relation between muscle physiology and muscle biochemistry.Ann. Rev. Physiol. 42, 293–309.
Eisenberg, E., Hill, T. &Chen, Y. (1980) Cross-bridge model of muscle contraction.Biophys. J. 29, 195–227.
Ferenczi, M. A., Simmons, R. M. &Sleep, J. A. (1982) General considerations of crossbridge models in relation to the dependence on MgATP concentration of mechanical parameters of skinned fibres from frog muscle. InBasic Biology of Muscles: A Comparative Approach (edited byTwarog, B. M., Levine, R. J. C. &Dewey, M. M.) pp. 91–107. New York: Raven Press.
Ferenczi, M. A., Goldman, Y. E. &Simmons, R. M. (1984) The dependence of force and shortening velocity on substrate concentration in skinned muscle fibres fromRana temporaria.J. Physiol., Lond. 350, 519–43.
Goldman, Y. E., Hibberd, M. G. &Trentham, D. R. (1984) Initiation of active contraction by photogeneration of adenosine-5′-triphosphate in rabbit psoas muscle fibres.J. Physiol., Lond. 354, 605–24.
Greene, L. E. &Eisenberg, E. (1980) Dissociation of the acin-subfragment 1 complex by adenyl-5′-yl imido-diphosphate, MgADP and PPi.J. biol. Chem. 251, 543–8.
Herzig, J. W., Peterson, J. W., Ruegg, J. C. &Solaro, R. J. (1981) Vanadate and phosphate ions reduce tension and increase cross-bridge kinetics in chemically skinned heart muscle.Biochem. Biophys. Acta 672, 191–6.
Hibberd, M. G., Dantzig, J. A., Trentham, D. R. &Goldman, Y. E. (1985) Phosphate release and force generation in skeletal muscle fibres.Science 228, 1317–9.
Hibberd, M. G. &Trentham, D. R. (1986) Relationships between chemical and mechanical events during muscular contraction.Ann. Rev. Biophys. Biophys. Chem. 15, 119–61.
Highsmith, S. (1977) The effect of temperature and salts on myosin subfragment-1 and F-actin association.Arch. Biochem. Biophys. 180, 404–8.
Hill, T. L. (1974) Theoretical formalism for the sliding filament model of contraction of striated muscle, part I.Prog. Biophys. Molec. Biol. 28, 267–340.
Huxley, A. F. (1957) Muscle structure and theories of contraction.Prog. Biophys. 7, 255–318.
Huxley, A. F. (1973) A note suggesting that the crossbridge attachment during muscle contraction may take place in two stages.Proc. R. Soc. B183, 83–6.
Huxley, A. F. &Simmons, R. M. (1971) Proposed mechanism of force generation in striated muscle.Nature 233, 533–8.
Julian, F. J. &Sollins, M. R. (1973) Regulation of force and speed of shortening in muscle contraction.Cold Spring Harbor Symp. Quant. Biol. 37, 637–45.
Kammermeier, H., Schmidt, P. &Jungling, E. (1982) Free energy change of ATP-hydrolysis: a causal factor of early hypoxic failure of the myocardium?J. molec. cell. Card. 14, 267–77.
Kawai, M. (1982) Correlation between experimental processes and cross-bridge kinetics. InBasic Biology of Muscles: A Comparative Approach (edited byTwarog, B. M., Levine, R. J. C. &Dewey, M. M.) pp. 109–130. New York: Raven Press.
Kawai, M. (1986) The role of orthophosphate in cross-bridge kinetics in chemically skinned rabbit psoas fibres as detected with sinusoidal and step length alterations.J. Musc. Res. Cell Motil. 7, 421–34.
Kawai, M., Guth, K., Winnikes, K., Haist, C. &Ruegg, J. C. (1987) The effect of inorganic phosphate on the ATP hydrolysis rate and the tension transients in chemically skinned rabbit psoas fibers.Pflügers Arch. ges. Physiol. 408, 1–9.
Kentish, J. C. (1986) The effects of inorganic phosphate and creatine phosphate in skinned muscles from rat ventricle.J. Physiol., Lond. 370, 585–604.
Kress, M., Huxley, H. E., Farugi, A. R. &Hendrix, J. (1986) Structural changes during activation of frog studied by time-resolved X-ray diffraction.J. molec. Biol. 188, 325–42.
Kushmerick, M. J. &Davies, R. E. (1969) The chemical energetics of muscle contraction. II. The chemistry, efficiency, and power of maximally working sartorious muscles.Proc. R. Soc. Lond. B174, 293–313.
Kushmerick, M. J. (1986) Lessons for muscle energetics from31P NMR spectroscopy.Adv. exp. Med. Biol. 194, 647–63.
Lacktis, J. W. &Homsher, E. (1987) The force response to photogenerated ADP in isometrically contracting glycerinated rabbit psoas muscle fibres.Biophys. J. 51, 475a.
Luney, D. J. E. &Godt, R. (1987) The effect of pH, ADP, inorganic phosphate (Pi) and affinity on the maximum velocity of shortening and force production of skinned rabbit muscle fibers.Biophys. J. 51, 468a.
Moss, R. L. (1982) The effect of calcium on the maximum velocity of shortening in skinned skeletal muscle fibres of the rabbit.J. Musc. Res. Cell Motil. 3, 295–311.
Nosek, T. M., Fender, K. Y. &Godt, R. E. (1987) It is diprotonated inorganic phosphate that depresses force in skinned skeletal muscle fibers.Science 236, 191–3.
Pate, E. &Cooke, R. (1985) The inhibition of muscle contraction by adenosine 5′(γ,-imido) triphosphate and by pyrophosphate.Biophys. J. 47, 773–80.
Pate, E. &Cooke, R. (1986) A model for the interaction of muscle cross-bridges with ligands which compete with ATP.J. Theor. Biol. 118, 215–30.
Podolsky, R. J., Noland, A. C. &Zaveler, S. A. (1969) Crossbridge properties derived from muscle isotonic velocity transients.Proc. natn. Acad. Sci. U.S.A. 64, 504–11.
Ruegg, J. C., Schadler, M., Steiger, G. J. &Miller, G. (1971) Effects of inorganic phosphate on the contractile mechanism.Pflügers Arch. ges. Physiol. 325, 359–64.
Schoenberg, M. &Wells, J. B. (1984) Stiffness, force and sarcomere shortening during a twitch in frog semitendinosus muscle bundles.Biophys. J. 45, 389–97.
Siemankowski, R. F., Wiseman, M. O. &White, H. W. (1985) ADP dissociation from actomyosin subfragment 1 is sufficiently slow to limit the unloaded shortening velocity in vertebrate muscle.Proc. natn. Acad. Sci. U.S.A. 82, 658–62.
Sleep, J. &Hutton, R. L. (1980) Exchange between inorganic phosphate and adenosine 5′-triphosphate in the medium by actomyosin subfragment 1.Biochemistry 19, 1276–83.
Sleep, J. &Glyn, H. (1986) Inhibition of myofibrillar and actomyosin subfragment 1 adenosinetriphosphatase by adenosine 5′-diphosphate and adenyl-5′-yl imidodiphosphate.Biochemistry 25, 1149–54.
Stein, L. A., Schwarz, R. P., Chock, P. B. &Eisenberg, E. (1979) Mechanism of actomyosin triphosphatase. Evidence that adenosine 5′-triphosphate hydrolysis can occur without dissociation of the actomyosin complex.Biochemistry 18, 3895–909.
Taylor, E. W. (1979) Mechanism of actomyosin ATPase and the problem of muscle contraction.CRC Crit. Rev. Biochem. 7, 103–64.
Thorson, J. &White, D. C. S. (1969) Distributed representation for actin-myosin interaction in the oscillatory contraction of muscle.Biophys. J. 9, 360–90.
Webb, M. R., Hibberd, M. G., Goldman, Y. E. &Trentham, D. R. (1986) Oxygen exchange between Pi in the medium and water during ATP hydrolysis mediated by skinned fibers from rabbit skeletal muscle. Evidence for Pi binding to a force-generating state.J. biol. Chem. 261, 15557–64.
White, D. C. S. &Thorson, J. (1972) Phosphate starvation and the nonlinear dynamics of insect fibrillar flight muscle.J. gen. Physiol. 60, 307–36.
White, H. D. &Taylor, E. W. (1976) Energetics and mechanism of actomyosin adenosine triphosphatase.Biochemistry 15, 5818–26.
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Pate, E., Cooke, R. A model of crossbridge action: the effects of ATP, ADP and Pi . J Muscle Res Cell Motil 10, 181–196 (1989). https://doi.org/10.1007/BF01739809
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DOI: https://doi.org/10.1007/BF01739809