Cellular dynamics of the SecA ATPase at the single molecule level

Publication Name

Scientific Reports

Abstract

In bacteria, the SecA ATPase provides the driving force for protein secretion via the SecYEG translocon. While the dynamic interplay between SecA and SecYEG in translocation is widely appreciated, it is not clear how SecA associates with the translocon in the crowded cellular environment. We use super-resolution microscopy to directly visualize the dynamics of SecA in Escherichia coli at the single-molecule level. We find that SecA is predominantly associated with and evenly distributed along the cytoplasmic membrane as a homodimer, with only a minor cytosolic fraction. SecA moves along the cell membrane as three distinct but interconvertible diffusional populations: (1) A state loosely associated with the membrane, (2) an integral membrane form, and (3) a temporarily immobile form. Disruption of the proton-motive-force, which is essential for protein secretion, re-localizes a significant portion of SecA to the cytoplasm and results in the transient location of SecA at specific locations at the membrane. The data support a model in which SecA diffuses along the membrane surface to gain access to the SecYEG translocon.

Open Access Status

This publication may be available as open access

Volume

11

Issue

1

Article Number

1433

Funding Sponsor

Stichting voor Fundamenteel Onderzoek der Materie

Share

COinS
 

Link to publisher version (DOI)

http://dx.doi.org/10.1038/s41598-021-81081-2