AI Article Synopsis
- MinD is an ATPase in E. coli that helps control cell division by preventing the assembly of division machinery at the cell's poles, ensuring it forms at the center instead.
- ClpXP, a bacterial proteasome complex, degrades MinD, particularly during the stationary phase when the cell is not dividing, thereby regulating its levels.
- The N-terminal region of MinD, especially residue Arg 3, is important for this degradation process, affecting MinC and MinD's structural assemblies and overall functionality during slower growth periods.
Article Abstract
MinD is a cell division ATPase in Escherichia coli that oscillates from pole to pole and regulates the spatial position of the cell division machinery. Together with MinC and MinE, the Min system restricts assembly of the FtsZ-ring to midcell, oscillating between the opposite ends of the cell and preventing FtsZ-ring misassembly at the poles. Here, we show that the ATP-dependent bacterial proteasome complex ClpXP degrades MinD in reconstituted degradation reactions in vitro and in vivo through direct recognition of the MinD N-terminal region. MinD degradation is enhanced during stationary phase, suggesting that ClpXP regulates levels of MinD in cells that are not actively dividing. ClpXP is a major regulator of growth phase-dependent proteins, and these results suggest that MinD levels are also controlled during stationary phase. In vitro, MinC and MinD are known to coassemble into linear polymers; therefore, we monitored copolymers assembled in vitro after incubation with ClpXP and observed that ClpXP promotes rapid MinCD copolymer destabilization and direct MinD degradation by ClpXP. The N terminus of MinD, including residue Arg 3, which is near the ATP-binding site in sequence, is critical for degradation by ClpXP. Together, these results demonstrate that ClpXP degradation modifies conformational assemblies of MinD in vitro and depresses Min function in vivo during periods of reduced proliferation.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7857489 | PMC |
| http://dx.doi.org/10.1074/jbc.RA120.013866 | DOI Listing |
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