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Reaction cycle membrane potential

FIGURE 19-9 IMADH ubiquinone oxidoreductase (Complex I). Complex I catalyzes the transfer of a hydride ion from NADH to FMN, from which two electrons pass through a series of Fe-S centers to the iron-sulfur protein N-2 in the matrix arm of the complex. Electron transfer from N-2 to ubiquinone on the membrane arm forms QH2, which diffuses into the lipid bilayer. This electron transfer also drives the expulsion from the matrix of four protons per pair of electrons. The detailed mechanism that couples electron and proton transfer in Complex I is not yet known, but probably involves a Q cycle similar to that in Complex III in which QH2 participates twice per electron pair (see Fig. 19-12). Proton flux produces an electrochemical potential across the inner mitochondrial membrane (N side negative, P side positive), which conserves some of the energy released by the electron-transfer reactions. This electrochemical potential drives ATP synthesis. [Pg.698]

Figure 18.39. Mechanism of Mitochondrial ATP-ADP Translocase. The translocase catalyzes the coupled entry of ADP and exit of ATP into and from the matrix. The reaction cycle is driven by membrane potential. The actual conformational change corresponding to eversion of the binding site could be quite small. Figure 18.39. Mechanism of Mitochondrial ATP-ADP Translocase. The translocase catalyzes the coupled entry of ADP and exit of ATP into and from the matrix. The reaction cycle is driven by membrane potential. The actual conformational change corresponding to eversion of the binding site could be quite small.
The gastric H,K ATPase is electroneutral, in contrast to the Na,K ATPase, because the number of H ions exported is the same as the number of K ions imported. However, each half of the reaction cycle generates an equal but opposite membrane potential as the ion traverses the membrane domain. [Pg.26]

The proton-motive Q-cycle model, put forward by Mitchell (references 80 and 81) and by Trumpower and co-workers, is invoked in the following manner (1) One electron is transferred from ubiquinol (ubiquinol oxidized to ubisemi-quinone see Figure 7.27) to the Rieske [2Fe-2S] center at the Qo site, the site nearest the intermembrane space or p side (2) this electron can leave the bci complex via an attached cytochrome c or be transferred to cytochrome Ci (3) the reactive ubisemiquinone reduces the low-potential heme bL located closer to the membrane s intermembrane (p) side (4) reduced heme bL quickly transfers an electron to high-potential heme bn near the membrane s matrix side and (5) ubiquinone or ubisemiquinone oxidizes the reduced bn at the Qi site nearest the matrix or n side. Proton translocation results from the deprotonation of ubiquinol at the Qo site and protonation of ubisemiquinone at the Qi site. Ubiquinol generated at the Qi site is reoxidized at the Qo site (see Figure 7.27). Additional protons are transported across the membrane from the matrix (see Figure 7.26 illustrating a similar process for cytochrome b(6)f). The overall reaction can be written... [Pg.395]

In purple photosynthetic bacteria, electrons return to P870+ from the quinones QA and QB via a cyclic pathway. When QB is reduced with two electrons, it picks up protons from the cytosol and diffuses to the cytochrome bct complex. Here it transfers one electron to an iron-sulfur protein and the other to a 6-type cytochrome and releases protons to the extracellular medium. The electron-transfer steps catalyzed by the cytochrome 6c, complex probably include a Q cycle similar to that catalyzed by complex III of the mitochondrial respiratory chain (see fig. 14.11). The c-type cytochrome that is reduced by the iron-sulfur protein in the cytochrome be, complex diffuses to the reaction center, where it either reduces P870+ directly or provides an electron to a bound cytochrome that reacts with P870+. In the Q cycle, four protons probably are pumped out of the cell for every two electrons that return to P870. This proton translocation creates an electrochemical potential gradient across the membrane. Protons move back into the cell through an ATP-synthase, driving the formation of ATP. [Pg.340]

Separation membranes can be extremely important to the economic success of the S-I cycle, as they can improve the overall efficiency of the cycle through removal of water, SO2, and H2 from the chemical stream. This can reduce the amount of excess heat needed to boil off the water and improve the conversion efficiency of decomposition reactions. There are three potential membrane applications within the S-I cycle ... [Pg.111]

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See also in sourсe #XX -- [ Pg.7 ]



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Cycles membranes

Cycling reactions

Membrane cycling

Membrane potential

Membrane reactions

Potential cycling

Reaction cycle

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