| The C-Terminal Domain of MinC Inhibits Assembly of the Z Ring in Escherichia coli � (2006) | |||||||||||||
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| regulates FtsZ assembly at the cell poles, helping to ensure that the Z ring will assemble only at midcell. Of the three Min proteins, MinC is sufficient to inhibit Z-ring assembly. By binding to MinD, which is mostly localized at the membrane near the cell poles, MinC is sequestered away from the cell midpoint, increasing the probability of Z-ring assembly there. Previously, it has been shown that the two halves of MinC have two distinct functions. The N-terminal half is sufficient for inhibition of FtsZ assembly, whereas the C-terminal half of the protein is required for binding to MinD as well as to a component of the division septum. In this study, we discovered that overproduction of the C-terminal half of MinC (MinC 122–231) could also inhibit cell division and that this inhibition was at the level of Z-ring disassembly and dependent on MinD. We also found that fusing green fluorescent protein to either the N-terminal end of MinC 122–231, the C terminus of full-length MinC, or the C terminus of MinC 122–231 perturbed MinC function, which may explain why cell division inhibition by MinC 122–231 was not detected previously. These results suggest that the C-terminal half of MinC has an additional function in the regulation of Z-ring assembly. MinC inhibits formation of the Z ring by preventing FtsZ assembly. However, the binding interactions between FtsZ and MinC are not well understood. MinC consists of two independent | |||||||||||||
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