C-terminal eYFP fusion impairs MinE function.

Open Biol

Faculty of Biology, Institute of Biology II, University of Freiburg, Schänzlestr. 1, 79104 Freiburg, Germany.

Published: May 2020

AI Article Synopsis

  • The Min system is crucial for the correct positioning of the septum ring during cell division by creating a concentration gradient that keeps MinD low at mid-cell.
  • MinE, when tagged with the enhanced yellow fluorescent protein (eYFP), loses its ability to effectively interact with MinD and MinC, hindering essential functions in the oscillation process.
  • Investigation indicates that the aggregation of MinE-eYFP and other fluorescent proteins could negatively affect multiple functions of MinE, suggesting widespread issues with fluorescent tagging in similar protein studies.

Article Abstract

The Min system plays an important role in the proper placement of the septum ring at mid-cell during cell division. MinE forms a pole-to-pole spatial oscillator with the membrane-bound ATPase MinD, resulting in MinD concentration being the lowest at mid-cell. MinC, the direct inhibitor of the septum initiator protein FtsZ, forms a complex with MinD at the membrane, mirroring its polar gradients. Therefore, MinC-mediated FtsZ inhibition occurs away from mid-cell. Min oscillations are often studied in living cells by time-lapse microscopy using fluorescently labelled Min proteins. Here, we show that, despite permitting oscillations to occur in a range of protein concentrations, the enhanced yellow fluorescent protein (eYFP) C-terminally fused to MinE impairs its function. Combining , and approaches, we demonstrate that eYFP compromises the ability of MinE to displace MinC from MinD, to stimulate MinD ATPase activity and to directly bind to the membrane. Moreover, we reveal that MinE-eYFP is prone to aggregation. analyses predict that other fluorescent proteins are also likely to compromise several functionalities of MinE, suggesting that the results presented here are not specific to eYFP.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7276532PMC
http://dx.doi.org/10.1098/rsob.200010DOI Listing

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