4.6 Article

PcoB is a defense outer membrane protein that facilitates cellular uptake of copper

期刊

PROTEIN SCIENCE
卷 31, 期 7, 页码 -

出版社

WILEY
DOI: 10.1002/pro.4364

关键词

gut microbiota; outer membrane protein structure; PcoB

资金

  1. Agnes og Poul Friis Fond
  2. Augustinus Fonden [16-1992]
  3. Carl Tryggers Stiftelse for Vetenskaplig Forskning [CTS 17:22, CTS 21:1773]
  4. Carlsbergfondet [2013_01_0641, CF15-0542]
  5. Crafoordska Stiftelsen [20170818, 20180652, 20200739]
  6. DanScatt
  7. Det Frie Forskningsrad [4183-00559, 6108-00479, 9039-00273]
  8. Hartmann Fonden [A29519]
  9. High-Performance Computing Center North (HPC2N) [SNIC 2018/2-32, SNIC 2019/2-29]
  10. Knut och Alice Wallenbergs Stiftelse [2015.0131, 2020.0194]
  11. Lundbeckfonden [R133-A12689, R313-2019-774]
  12. National Institute of General Medical Sciences [R35GM128704]
  13. Novo Nordisk Fonden [NNF13OC0007471]
  14. Per-Eric and Ulla Schyberg Foundation [38267]
  15. Vera og Carl Johan Michaelsens Legat [2016-04474, 2020-03840, 521-2012-2243]
  16. Welch Foundation [AT1935-20170325, AT-2073-20210327]

向作者/读者索取更多资源

The study characterizes the structure and function of the outer membrane component PcoB in the Pco system, revealing its role in ion-conducting pathway and a potential unorthodox defense mechanism against metal stress.
Copper (Cu) is one of the most abundant trace metals in all organisms, involved in a plethora of cellular processes. Yet elevated concentrations of the element are harmful, and interestingly prokaryotes are more sensitive for environmental Cu stress than humans. Various transport systems are present to maintain intracellular Cu homeostasis, including the prokaryotic plasmid-encoded multiprotein pco operon, which is generally assigned as a defense mechanism against elevated Cu concentrations. Here we structurally and functionally characterize the outer membrane component of the Pco system, PcoB, recovering a 2.0 angstrom structure, revealing a classical beta-barrel architecture. Unexpectedly, we identify a large opening on the extracellular side, linked to a considerably electronegative funnel that becomes narrower towards the periplasm, defining an ion-conducting pathway as also supported by metal binding quantification via inductively coupled plasma mass spectrometry and molecular dynamics (MD) simulations. However, the structure is partially obstructed towards the periplasmic side, and yet flux is permitted in the presence of a Cu gradient as shown by functional characterization in vitro. Complementary in vivo experiments demonstrate that isolated PcoB confers increased sensitivity towards Cu. Aggregated, our findings indicate that PcoB serves to permit Cu import. Thus, it is possible the Pco system physiologically accumulates Cu in the periplasm as a part of an unorthodox defense mechanism against metal stress. These results point to a previously unrecognized principle of maintaining Cu homeostasis and may as such also assist in the understanding and in efforts towards combatting bacterial infections of Pco-harboring pathogens.

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