Activation of Striated Muscle: Nearest-neighbor Regulatory-unit and Cross-bridge Influence on Myofilament Kinetics

We have formulated a three-compartment model of muscle activation that includes both strong cross-bridge (XB) and Ca 2+-activated regulatory-unit (RU) mediated nearest-neighbor cooperative influences. The model is based on the tight coupling premise—that XB retain activating Ca 2+ on the thin filame...

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Veröffentlicht in:Journal of molecular biology 2002-10, Vol.322 (5), p.1065-1088
Hauptverfasser: Robinson, John M., Wang, Ying, Kerrick, W.Glenn L., Kawai, Ryoichi, Cheung, Herbert C.
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Sprache:eng
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Zusammenfassung:We have formulated a three-compartment model of muscle activation that includes both strong cross-bridge (XB) and Ca 2+-activated regulatory-unit (RU) mediated nearest-neighbor cooperative influences. The model is based on the tight coupling premise—that XB retain activating Ca 2+ on the thin filament. Using global non-linear least-squares, the model produced excellent fits to experimental steady-state force-pCa and ATPase-pCa data from skinned rat soleus fibers. In terms of the model, nearest-neighbor influences over the range of Ca 2+ required for activation cause the Ca 2+ dissociation rate from regulatory-units ( k off) to decrease and the cross-bridge association rate ( f) to increase each more than ten-fold. Moreover, the rate variations occur in separate Ca 2+ regimes. The energy of activation governing f is strongly influenced by both neighboring RU and XB. In contrast, the energy of activation governing k off is less affected by neighboring XB than by neighboring RU. Nearest-neighbor cooperative influences provide both an overall sensitization to Ca 2+ and the well-known steep response of force to free Ca 2+. The apparent sensitivity for Ca 2+-activation of force and ATPase is a function of cross-bridge kinetic rates. The model and derived parameter set produce simulated behavior in qualitative agreement with steady-state experiments reported in the literature for partial TnC replacement, increased [P i], increased [ADP], and MalNEt-S1 addition. The model is an initial attempt to construct a general theory of striated muscle activation—one that can be consistently used to interpret data from various types of muscle manipulation experiments.
ISSN:0022-2836
1089-8638
DOI:10.1016/S0022-2836(02)00855-0