Literature DB >> 3417649

An activation-collision mechanism for cholesterol transfer between membranes.

T L Steck1, F J Kezdy, Y Lange.   

Abstract

We report the results of experiments which show that cholesterol transfer between membranes cannot proceed by aqueous diffusion, as widely held, but must involve a more complex mechanism. (a) The rate of transfer of [3H]cholesterol from red blood cells was found to vary inversely with the size of the acceptor particle (ghosts, vesicles of ghosts, liposomes, and plasma lipoproteins). (b) The transfer of [3H]cholesterol from red blood cells to ghosts was accelerated by the presence of plasma, even though the plasma competed with the ghosts as an acceptor. (c) The rate of transfer of [3H]cholesterol from red blood cells to ghosts decreased to zero with increasing dilution but was not simply second-order. (d) The cholesterol in retinal rod disc membranes is not at equilibrium with plasma lipoproteins in that disc cholesterol increased when the homogenates were incubated in vitro with plasma. (e) The kinetics of cholesterol transfer cannot be limited by unstirred layer effects since the transfer of lysolecithin in the same system was faster than that of cholesterol by 3 orders of magnitude. The simplest model compatible with all the data suggests a two-step pathway involving a first-order followed by a second-order process. The first step could be a unimolecular activation event, perhaps the movement of the sterol in the donor particle to a more exposed (hydrated) position. In the second step, the activated sterol would be transferred during transient collisions between donor and acceptor particles. When collision is not rate-limiting, the overall process would appear to be simply first-order, hence kinetically indistinguishable from the aqueous diffusion mechanism. The activation-collision model thus not only rationalizes our data but is also consistent with the simpler kinetics previously reported for the transfer of both membrane phospholipids and sterols.

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Year:  1988        PMID: 3417649

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  14 in total

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2.  No Evidence for Spontaneous Lipid Transfer at ER-PM Membrane Contact Sites.

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Review 4.  Use of cyclodextrins to manipulate plasma membrane cholesterol content: evidence, misconceptions and control strategies.

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5.  Probing red cell membrane cholesterol movement with cyclodextrin.

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6.  Cholesterol increase in mitochondria: its effect on inner-membrane functions, submitochondrial localization and ultrastructural morphology.

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Review 7.  Cholesterol homeostasis and the escape tendency (activity) of plasma membrane cholesterol.

Authors:  Yvonne Lange; Theodore L Steck
Journal:  Prog Lipid Res       Date:  2008-03-29       Impact factor: 16.195

8.  Genetic, anatomic, and clinical determinants of human serum sterol and vitamin D levels.

Authors:  Ashlee R Stiles; Julia Kozlitina; Bonne M Thompson; Jeffrey G McDonald; Kevin S King; David W Russell
Journal:  Proc Natl Acad Sci U S A       Date:  2014-09-08       Impact factor: 11.205

9.  Transport of sterols to the plasma membrane of leek seedlings

Authors: 
Journal:  Plant Physiol       Date:  1998-07       Impact factor: 8.340

10.  Two-photon time-lapse microscopy of BODIPY-cholesterol reveals anomalous sterol diffusion in chinese hamster ovary cells.

Authors:  Frederik W Lund; Michael A Lomholt; Lukasz M Solanko; Robert Bittman; Daniel Wüstner
Journal:  BMC Biophys       Date:  2012-10-18       Impact factor: 4.778

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