The peptidoglycan (PG) sacculus is composed of long glycan strands cross-linked together by short peptides forming a covalently closed meshwork that protects the bacterial cell from osmotic lysis and specifies its shape. PG hydrolases play essential roles in remodeling this three-dimensional network during growth and division but how these autolytic enzymes are regulated remains poorly understood. The FtsEX ABC transporter-like complex has emerged as a broadly conserved regulatory module in controlling cell wall hydrolases in diverse bacterial species. In most characterized examples, this complex regulates distinct PG hydrolases involved in cell division and is intimately associated with the cytokinetic machinery called the divisome. However, in the gram-positive bacterium Bacillus subtilis the FtsEX complex is required for cell wall elongation where it regulates the PG hydrolase CwlO that acts along the lateral cell wall. To investigate whether additional factors are required for FtsEX function outside the divisome, we performed a synthetic lethal screen taking advantage of the conditional essentiality of CwlO. This screen identified two uncharacterized factors (SweD and SweC) that are required for CwlO activity. We demonstrate that these proteins reside in a membrane complex with FtsX and that amino acid substitutions in residues adjacent to the ATPase domain of FtsE partially bypass the requirement for them. Collectively our data indicate that SweD and SweC function as essential co-factors of FtsEX in controlling CwlO during cell wall elongation. We propose that factors analogous to SweDC function to support FtsEX activity outside the divisome in other bacteria. Author summary Bacterial growth and division require the synthesis and remodeling of the cell wall exoskeleton. To prevent lethal breaches in this protective layer, peptidoglycan (PG) hydrolases that remodel the cell wall must be carefully regulated but the mechanisms underlying this control remain poorly understood. The noncanonical ABC transporter FtsEX has emerged as a broadly conserved regulator of PG hydrolases. In most characterized examples, FtsEX is integrated into the division machinery where it controls cell wall cleavage during cytokinesis. By contrast, in Bacillus subtilis the FtsEX complex functions in cell wall elongation. Here, we report the identification of two previously uncharacterized proteins (SweD and SweC) that function as essential co-factors of FtsEX in controlling PG hydrolase activity along the lateral cell wall. Homologs of SweD and SweC are found in a subset of firmicutes. We propose that these and analogous factors enable FtsEX to function outside the divisome to control cell wall elongation hydrolases.
【초록키워드】 peptide, Bacillus subtilis, Regulatory, Protein, peptides, Control, membrane, cleavage, Bacteria, synthesis, mechanism, function, Protective, Amino acid, regulate, amino acid substitutions, the cell, bacterial cell, cell wall, cell division, gram-positive bacterium, autolytic enzymes, Support, Hydrolases, Factor, enzyme, growth, Author, complex, residue, hydrolase, domain, residues, remodeling, bacterial species, division, peptidoglycan, homologs, gram, sacculus, cytokinesis, divisome, firmicutes, osmotic lysis, ATPase, amino acid substitution, Prevent, Cell, PROTECT, performed, conserved, involved, composed, required, characterized, regulated, subset, control cell, ABC, 【제목키워드】 cell wall, complex, Cell,