Abstract

Lipopolysaccharide (LPS) is an essential glycolipid that covers the surface of gram-negative bacteria. The transport of LPS involves a dedicated seven-protein transporter system called the lipopolysaccharide transport system (Lpt) machinery that physically spans the entire cell envelope. The LptB2FG complex is an ABC transporter that hydrolyzes ATP to extract LPS from the inner membrane for transport to the outer membrane. Here, we extracted LptB2FG directly from the inner membrane with its original lipid environment using styrene-maleic acid polymers. We found that styrene-maleic acid polymers–LptB2FG in nanodiscs display not only ATPase activity but also a previously uncharacterized adenylate kinase (AK) activity, as it catalyzed phosphotransfer between two ADP molecules to generate ATP and AMP. The ATPase and AK activities of LptB2FG were both stimulated by the interaction on the periplasmic side with the periplasmic LPS transport proteins LptC and LptA and inhibited by the presence of the LptC transmembrane helix. We determined that the isolated ATPase module (LptB) had weak AK activity in the absence of transmembrane proteins LptF and LptG, and one mutation in LptB that weakens its affinity for ADP led to AK activity similar to that of fully assembled complex. Thus, we conclude that LptB2FG is capable of producing ATP from ADP, depending on the assembly of the Lpt bridge, and that this AK activity might be important to ensure efficient LPS transport in the fully assembled Lpt system.

Highlights

  • Gram-negative bacteria possess a doubleATP hydrolysis relaxes the dimer into an open conformation

  • LptB2FG associates with LptC via 2 distinct interactions: i) LptF/LptG interact with LptC transmembrane domain, which contributes to form the cavity that accommodates LPS into the complex and regulates LptB2FG ATPase activity [6], ii) LptF and LptC jellyroll domains associate in the periplasm

  • The superfamily of an binding Cassette (ABC) transporter proteins comprises more than 500 members, and supports traffic of metabolites and molecules through ATP hydrolysis [7]

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Summary

Introduction

Gram-negative bacteria possess a doubleATP hydrolysis relaxes the dimer into an open conformation. The ATPase and AK activities of LptB2FG were both stimulated by the interaction on the periplasmic side with the periplasmic LPS transport proteins LptC and LptA and inhibited by the presence of the LptC transmembrane helix. 1H NMR on nucleotides showed the a continuous flow of LPS molecules needs to SMA-LptB2FG complex has ATPase activity but cross the periplasm and reach the external layer to Adenylate Kinase (AK) activity, and both keep up with cell growth.

Results
Conclusion

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