Kinetic advantage of forming respiratory supercomplexes

https://doi.org/10.1016/j.bbabio.2020.148193Get rights and content
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Highlights

  • The electron flux through complexes III and IV can be limited by diffusion of cyt c.

  • The electron flux is determined by the equilibration time of cyt c in the water space.

  • Under realistic conditions there is a kinetic advantage in forming III-IV supercomplexes.

Abstract

Components of respiratory chains in mitochondria and some aerobic bacteria assemble into larger, multiprotein membrane-bound supercomplexes. Here, we address the functional significance of supercomplexes composed of respiratory-chain complexes III and IV. Complex III catalyzes oxidation of quinol and reduction of water-soluble cytochrome c (cyt c), while complex IV catalyzes oxidation of the reduced cyt c and reduction of dioxygen to water. We focus on two questions: (i) under which conditions does diffusion of cyt c become rate limiting for electron transfer between these two complexes? (ii) is there a kinetic advantage of forming a supercomplex composed of complexes III and IV? To answer these questions, we use a theoretical approach and assume that cyt c diffuses in the water phase while complexes III and IV either diffuse independently in the two dimensions of the membrane or form supercomplexes. The analysis shows that the electron flux between complexes III and IV is determined by the equilibration time of cyt c within the volume of the intermembrane space, rather than the cyt c diffusion time constant. Assuming realistic relative concentrations of membrane-bound components and cyt c and that all components diffuse independently, the data indicate that electron transfer between complexes III and IV can become rate limiting. Hence, there is a kinetic advantage of bringing complexes III and IV together in the membrane to form supercomplexes.

Keywords

Electron transfer
Proton transfer
Cytochrome aa3
Membrane protein
Ligand
Kinetics
Mechanism

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