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From protons to OXPHOS supercomplexes and Alzheimer's disease: Structure-dynamics-function relationships of energy-transducing membranes
Authors:H Seelert  DN Dani  T Hauß  F Krause  M Frenzel  S Rexroth  HJ Schwaßmann  J Vonck
Institution:a Physical Biochemistry, Department of Chemistry, Technische Universität Darmstadt, Petersenstrasse 22, D-64287 Darmstadt, Germany
b Helmholtz-Zentrum Berlin für Materialien und Energie, Lise-Meitner-Campus, Glienicker Strasse 100, D-14109 Berlin, Germany
c Max Planck Institute of Biophysics, Max-von-Laue-Strasse 3, D-60438 Frankfurt am Main, Germany
Abstract:By the elucidation of high-resolution structures the view of the bioenergetic processes has become more precise. But in the face of these fundamental advances, many problems are still unresolved. We have examined a variety of aspects of energy-transducing membranes from large protein complexes down to the level of protons and functional relevant picosecond protein dynamics. Based on the central role of the ATP synthase for supplying the biological fuel ATP, one main emphasis was put on this protein complex from both chloroplast and mitochondria. In particular the stoichiometry of protons required for the synthesis of one ATP molecule and the supramolecular organisation of ATP synthases were examined. Since formation of supercomplexes also concerns other complexes of the respiratory chain, our work was directed to unravel this kind of organisation, e.g. of the OXPHOS supercomplex I1III2IV1, in terms of structure and function. Not only the large protein complexes or supercomplexes work as key players for biological energy conversion, but also small components as quinones which facilitate the transfer of electrons and protons. Therefore, their location in the membrane profile was determined by neutron diffraction. Physico-chemical features of the path of protons from the generators of the electrochemical gradient to the ATP synthase, as well as of their interaction with the membrane surface, could be elucidated by time-resolved absorption spectroscopy in combination with optical pH indicators. Diseases such as Alzheimer's dementia (AD) are triggered by perturbation of membranes and bioenergetics as demonstrated by our neutron scattering studies.
Keywords:AFM  atomic force microscopy  AD  Alzheimer's disease    amyloid-β peptide  BN  blue-native  BR  bacteriorhodopsin  CBBG-250  Coomassie Brilliant Blue G-250  CF1FO  chloroplast ATP synthase  (C)FO  membrane integral part of the (chloroplast) ATP synthase  CHAPS  3-[3(cholamidopropyl)dimethylammonio]-1-propanesulfonate  CL  cardiolipin  CN  colourless native/clear native  CoQ10  ubiquinone  DIGE  difference gel electrophoresis  F1  hydrophilic part of the ATP synthase  OXPHOS  oxidative phosphorylation  PM  purple membrane  QENS  quasielastic neutron scattering  ROS  reactive oxygen species  ULV  unilamellar vesicles
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