4.5 Article

Proton diffusion along biological membranes

期刊

JOURNAL OF PHYSICS-CONDENSED MATTER
卷 23, 期 23, 页码 -

出版社

IOP Publishing Ltd
DOI: 10.1088/0953-8984/23/23/234103

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资金

  1. Russian Foundation for Basic Research [08-03-00094-a]
  2. NSF [PHY 0646273]
  3. NIH [GM54052]

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Biological surfaces are known to be capable of retaining protons and facilitating their lateral diffusion. Since the surface dynamically exchanges protons with the bulk, the proton movement from a source to a target at the surface acquires a complicated pattern of coupled surface and bulk (2D + 3D) diffusion of which the main feature is that the surface acts as a proton-collecting antenna enhancing the proton flux from the bulk. A phenomenological model of this process is reviewed and its applications to recent experiments on lipid bilayers and small unilaminar vesicles are discussed. The model (i) introduces the important notions of the fast and slow regimes of proton exchange between the surface and the bulk, (ii) permits evaluation of the antenna radius and amplification coefficient in both regimes, (iii) explains the observed macroscopically large distances (in the micrometer range; Antonenko and Pohl 1998 FEBS Lett. 429 197) that the proton can travel along lipid membranes embedded into pure aqueous solutions, and (iv) predicts the dependence of the steady-state proton flux and the kinetics of the non-stationary diffusion upon the buffer concentration in buffered solutions. The surface diffusion coefficient for small unilaminar vesicles is calculated from experimental data (Sanden et al 2010 Proc. Natl Acad. Sci. USA 107 4129) to be 1 x 10(-5) cm(2) s(-1). The dependence of the shape of the kinetic curves representing protonation/deprotonation of a lipid-bound pH-sensitive dye attached to a planar bilayer lipid membrane upon the buffer concentration (Serowy et al 2003 Biophys. J. 84 1031) and the effect of changing the membrane composition (Antonenko and Pohl 2008 Eur. Biophys. J. 37 865) are explained.

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