Exercise and fatigue: integrating the role of K+, Na+ and Cl− in the regulation of sarcolemmal excitability of skeletal muscle (original) (raw)
2023, European Journal of Applied Physiology
Perturbations in K + have long been considered a key factor in skeletal muscle fatigue. However, the exercise-induced changes in K + intra-to-extracellular gradient is by itself insufficiently large to be a major cause for the force decrease during fatigue unless combined to other ion gradient changes such as for Na +. Whilst several studies described K +-induced force depression at high extracellular [K + ] ([K + ] e), others reported that small increases in [K + ] e induced potentiation during submaximal activation frequencies, a finding that has mostly been ignored. There is evidence for decreased Cl − ClC-1 channel activity at muscle activity onset, which may limit K +-induced force depression, and large increases in ClC-1 channel activity during metabolic stress that may enhance K + induced force depression. The ATP-sensitive K + channel (K ATP channel) is also activated during metabolic stress to lower sarcolemmal excitability. Taking into account all these findings, we propose a revised concept in which K + has two physiological roles: (1) K +-induced potentiation and (2) K +-induced force depression. During low-moderate intensity muscle contractions, the K +-induced force depression associated with increased [K + ] e is prevented by concomitant decreased ClC-1 channel activity, allowing K +-induced potentiation of sub-maximal tetanic contractions to dominate, thereby optimizing muscle performance. When ATP demand exceeds supply, creating metabolic stress, both K ATP and ClC-1 channels are activated. K ATP channels contribute to force reductions by lowering sarcolemmal generation of action potentials, whilst ClC-1 channel enhances the force-depressing effects of K + , thereby triggering fatigue. The ultimate function of these changes is to preserve the remaining ATP to prevent damaging ATP depletion.
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