AI Article Synopsis
- Type III Secretion Systems (T3SS) are crucial for transporting bacterial proteins, either for assembly into surface structures or directly into host cells.
- The FlhAB-FliPQR export gate controls protein entry and maintains cell membrane integrity, with specific residues in the FliR plug playing a key role in keeping the gate closed.
- Gate opening occurs in response to export signals from substrates and relies on energy from FlhA, while distinct signals from FliJ and the substrate are essential for efficient operation.
Article Abstract
Type III Secretion Systems (T3SS) transport proteins from the bacterial cytosol for assembly into cell surface nanomachines or direct delivery into target eukaryotic cells. At the core of the flagellar T3SS, the FlhAB-FliPQR export gate regulates protein entry into the export channel whilst maintaining the integrity of the cell membrane. Here, we identify critical residues in the export gate FliR plug that stabilise the closed conformation, preserving the membrane permeability barrier, and we show that the gate opens and closes in response to export substrate availability. Our data indicate that FlhAB-FliPQR gate opening, which is triggered by substrate export signals, is energised by FlhA in a proton motive force-dependent manner. We present evidence that the export substrate and the FliJ stalk of the flagellar ATPase provide mechanistically distinct, non-redundant gate-activating signals that are critical for efficient export.
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| http://dx.doi.org/10.1111/febs.16294 | DOI Listing |
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