Literature DB >> 21710299

Obstructed metabolite diffusion within skeletal muscle cells in silico.

Mayis K Aliev1, Alexander N Tikhonov.   

Abstract

Using a Monte Carlo simulation technique, we have modeled 3D diffusion of low molecular weight metabolites inside a skeletal muscle cell. The following structural elements are considered: (i) a regular lattice of actin and myosin filaments inside a myofibril, (ii) the membranes of sarcoplasmic reticulum and mitochondria surrounding the myofibrils, (iii) a set of myofibrils inside a skeletal muscle cell encircled by the outer cell membrane, and (iv) an additional set of regular intracellular structures ("macrocompartments") embedded into the cell interior. The macrocompartments are considered to simulate diffusion restrictions because of hypothetical cylindrical structures (16-22 μm in diameter) suggested earlier (de Graaf et al. Biophys J 78: 1657-1664, 2000). This model allowed us to calculate the apparent coefficients of particle diffusion in the radial and axial directions, D(app)(⊥) and D(app)(II), respectively. Particle movements in the axial direction are considered, at first approximation, as unrestricted diffusion (D(app)(II) = const). The apparent coefficient of radial diffusion, D(app)(⊥), decreases with time because of particle collisions with myofilaments and other rigid obstacles. Results of our random walk simulations are in fairly good agreement with experimental data on NMR measurements of restricted radial diffusion of phosphocreatine in white and red skeletal muscles of goldfish (Kinsey et al. NMR Biomed 12:1-7, 1999). Particle reflections from the low-permeable borders of macrocompartments (efficient diameter, D(eff)(MC) ≈ 9.2-10.4 μm) are the prerequisite for agreeing theoretical and experimental data. The low-permeable coverage of hypothetical macrocompartments (99.8% of coverage) provides the main contribution to time-dependent decrease in D(app)(⊥).

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Year:  2011        PMID: 21710299     DOI: 10.1007/s11010-011-0926-y

Source DB:  PubMed          Journal:  Mol Cell Biochem        ISSN: 0300-8177            Impact factor:   3.396


  56 in total

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Authors:  P R Shorten; J Sneyd
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5.  Compartmentalized energy transfer in cardiomyocytes: use of mathematical modeling for analysis of in vivo regulation of respiration.

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6.  Do laser diffraction studies on striated muscle indicate stepwise sarcomere shortening?

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7.  Technique for stabilizing the striation pattern in maximally calcium-activated skinned rabbit psoas fibers.

Authors:  B Brenner
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Authors:  A Partikian; B Olveczky; R Swaminathan; Y Li; A S Verkman
Journal:  J Cell Biol       Date:  1998-02-23       Impact factor: 10.539

9.  Mitochondria-cytoskeleton interaction: distribution of β-tubulins in cardiomyocytes and HL-1 cells.

Authors:  Rita Guzun; Minna Karu-Varikmaa; Marcela Gonzalez-Granillo; Andrey V Kuznetsov; Lauriane Michel; Cécile Cottet-Rousselle; Merle Saaremäe; Tuuli Kaambre; Madis Metsis; Michael Grimm; Charles Auffray; Valdur Saks
Journal:  Biochim Biophys Acta       Date:  2011-02-04

10.  Evaluation of restricted diffusion in cylinders. Phosphocreatine in rabbit leg muscle.

Authors:  P van Gelderen; D DesPres; P C van Zijl; C T Moonen
Journal:  J Magn Reson B       Date:  1994-03
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