4.7 Article

Cardiolipin is required in vivo for the stability of bacterial translocon and optimal membrane protein translocation and insertion

Journal

SCIENTIFIC REPORTS
Volume 10, Issue 1, Pages -

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41598-020-63280-5

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Funding

  1. NATO Science for Peace and Security Programme [SPS 985291]
  2. European Union's Horizon 2020 Research and Innovation programme under the Marie Skodowska-Curie grant [690853]
  3. Program of Competitive Growth of Kazan Federal University
  4. National Institutes of General Medical Sciences Grant [GM121493]
  5. John S. Dunn Foundation

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Translocation of preproteins across the Escherichia coli inner membrane requires anionic lipids by virtue of their negative head-group charge either in vivo or in situ. However, available results do not differentiate between the roles of monoanionic phosphatidylglycerol and dianionic cardiolipin (CL) in this essential membrane-related process. To define in vivo the molecular steps affected by the absence of CL in protein translocation and insertion, we analyzed translocon activity, SecYEG stability and its interaction with SecA in an E. coli mutant devoid of CL. Although no growth defects were observed, co- and post-translational translocation of alpha -helical proteins across inner membrane and the assembly of outer membrane beta -barrel precursors were severely compromised in CL-lacking cells. Components of proton-motive force which could impair protein insertion into and translocation across the inner membrane, were unaffected. However, stability of the dimeric SecYEG complex and oligomerization properties of SecA were strongly compromised while the levels of individual SecYEG translocon components, SecA and insertase YidC were largely unaffected. These results demonstrate that CL is required in vivo for the stability of the bacterial translocon and its efficient function in co-translational insertion into and translocation across the inner membrane of E. coli.

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