4.8 Article

Structure of the bc1-cbb3 respiratory supercomplex from Pseudomonas aeruginosa

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NATL ACAD SCIENCES
DOI: 10.1073/pnas.2307093120

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respiratory supercomplexes; cryoEM; structure; Pseudomonas aeruginosa; electron transport

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Energy conversion through electron transport chains is essential for ATP synthesis and membrane transport. The structure of a respiratory supercomplex (SC) formed between cytochrome bc1 and cytochrome cbb3 in the opportunistic pathogen Pseudomonas aeruginosa has been determined, revealing the involvement of intermediate electron carriers. Different isoforms of cytochrome cbb3 can also participate in SC formation, allowing the bacterium to adapt to different environmental conditions.
Energy conversion by electron transport chains occurs through the sequential transfer of electrons between protein complexes and intermediate electron carriers, creating the proton motive force that enables ATP synthesis and membrane transport. These protein complexes can also form higher order assemblies known as respiratory supercomplexes (SCs). The electron transport chain of the opportunistic pathogen Pseudomonas aerug-inosa is closely linked with its ability to invade host tissue, tolerate harsh conditions, and resist antibiotics but is poorly characterized. Here, we determine the structure of a P. aeruginosa SC that forms between the quinol:cytochrome c oxidoreductase (cytochrome bc1) and one of the organism's terminal oxidases, cytochrome cbb3, which is found only in some bacteria. Remarkably, the SC structure also includes two intermediate electron car-riers: a diheme cytochrome c4 and a single heme cytochrome c5. Together, these proteins allow electron transfer from ubiquinol in cytochrome bc1 to oxygen in cytochrome cbb3. We also present evidence that different isoforms of cytochrome cbb3 can participate in formation of this SC without changing the overall SC architecture. Incorporating these different subunit isoforms into the SC would allow the bacterium to adapt to different environmental conditions. Bioinformatic analysis focusing on structural motifs in the SC suggests that cytochrome bc1-cbb3 SCs also exist in other bacterial pathogens.

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