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Molecules in motion: influences of diffusion on metabolic structure and function in skeletal muscle

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TLDR
Experimental measurements of metabolic fluxes, diffusion distances and diffusion coefficients, coupled with reaction–diffusion mathematical models in a range of muscle types has started to reveal some general principles guiding muscle structure and metabolic function.
Abstract
Metabolic processes are often represented as a group of metabolites that interact through enzymatic reactions, thus forming a network of linked biochemical pathways. Implicit in this view is that diffusion of metabolites to and from enzymes is very fast compared with reaction rates, and metabolic fluxes are therefore almost exclusively dictated by catalytic properties. However, diffusion may exert greater control over the rates of reactions through: (1) an increase in reaction rates; (2) an increase in diffusion distances; or (3) a decrease in the relevant diffusion coefficients. It is therefore not surprising that skeletal muscle fibers have long been the focus of reaction–diffusion analyses because they have high and variable rates of ATP turnover, long diffusion distances, and hindered metabolite diffusion due to an abundance of intracellular barriers. Examination of the diversity of skeletal muscle fiber designs found in animals provides insights into the role that diffusion plays in governing both rates of metabolic fluxes and cellular organization. Experimental measurements of metabolic fluxes, diffusion distances and diffusion coefficients, coupled with reaction–diffusion mathematical models in a range of muscle types has started to reveal some general principles guiding muscle structure and metabolic function. Foremost among these is that metabolic processes in muscles do, in fact, appear to be largely reaction controlled and are not greatly limited by diffusion. However, the influence of diffusion is apparent in patterns of fiber growth and metabolic organization that appear to result from selective pressure to maintain reaction control of metabolism in muscle.

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The structural and functional coordination of glycolytic enzymes in muscle: evidence of a metabolon?

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References
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Journal ArticleDOI

Capillarisation, oxygen diffusion distances and mitochondrial content of carp muscles following acclimation to summer and winter temperatures.

TL;DR: Increases in the mitochondrial compartment with cold acclimation were accompanied by an increase in the capillary supply to both fast and slow muscles, and factors regulating thermal compensation of aerobic metabolism and the plasticity of fish muscle to environmental change are briefly discussed.
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Diffusional anisotropy is induced by subcellular barriers in skeletal muscle.

TL;DR: This work is the first example of diffusional anisotropy induced by readily identifiable intracellular structures, and the sarcoplasmic reticulum and mitochondria appear to be the principal intrACEllular structures that inhibit mobility in an orientation‐dependent manner.
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Nuclear magnetic resonance spectroscopy study of muscle growth, mdx dystrophy and glucocorticoid treatments: correlation with repair.

TL;DR: 1 H NMR is a reliable tool in the objective investigation of muscle repair status during muscular dystrophy, and is focused on monitoring muscle repair, not degeneration.
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A model for intracellular energy transport.

TL;DR: A viable alternative to the traditional Krogh model is presented which takes into account the inhomogeneity of the diffusion pathway as a result of mitochondrial clustering.
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In vivo NMR diffusion spectroscopy: 31P application to phosphorus metabolites in muscle

TL;DR: It is demonstrated that the displacement of phosphocreatine resembles free diffusion for short diffusion times but becomes limited as a result of boundaries due to compartmenta‐tion for longer diffusion times, indicating that phosphocreatingine moves freely in the cytosol but is limited by the boundaries of the muscle cells.
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