4.7 Article

Serial femtosecond crystallography structure of cytochrome c oxidase at room temperature

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SCIENTIFIC REPORTS
卷 7, 期 -, 页码 -

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NATURE PUBLISHING GROUP
DOI: 10.1038/s41598-017-04817-z

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资金

  1. X-ray Free-Electron Laser Priority Strategy Program (MEXT)
  2. Swedish Research Council [2015-00560, 349-2011-6485]
  3. Swedish Foundation for Strategic Research [SRL10-0036]
  4. Knut and Alice Wallenberg Foundation [KAW 2012.0284, KAW 2014.0275]
  5. European commission Marie Curie Training Networks
  6. Swedish Foundation for Strategic Research (SSF) [SRL10-0036] Funding Source: Swedish Foundation for Strategic Research (SSF)
  7. Swedish Research Council [2015-00560] Funding Source: Swedish Research Council

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Cytochrome c oxidase catalyses the reduction of molecular oxygen to water while the energy released in this process is used to pump protons across a biological membrane. Although an extremely well-studied biological system, the molecular mechanism of proton pumping by cytochrome c oxidase is still not understood. Here we report a method to produce large quantities of highly diffracting microcrystals of ba(3)-type cytochrome c oxidase from Thermus thermophilus suitable for serial femtosecond crystallography. The room-temperature structure of cytochrome c oxidase is solved to 2.3 angstrom resolution from data collected at an X-ray Free Electron Laser. We find overall agreement with earlier X-ray structures solved from diffraction data collected at cryogenic temperature. Previous structures solved from synchrotron radiation data, however, have shown conflicting results regarding the identity of the active-site ligand. Our room-temperature structure, which is free from the effects of radiation damage, reveals that a single-oxygen species in the form of a water molecule or hydroxide ion is bound in the active site. Structural differences between the ba(3)-type and aa(3)-type cytochrome c oxidases around the proton-loading site are also described.

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