Structures of a FtsZ single protofilament and a double-helical tube in complex with a monobody.
Junso FujitaHiroshi AmesakaTakuya YoshizawaKota HibinoNatsuki KamimuraNatsuko KurodaTakamoto KonishiYuki KatoMizuho HaraTsuyoshi InoueKeiichi NambaShun-Ichi TanakaHiroyoshi MatsumuraPublished in: Nature communications (2023)
FtsZ polymerizes into protofilaments to form the Z-ring that acts as a scaffold for accessory proteins during cell division. Structures of FtsZ have been previously solved, but detailed mechanistic insights are lacking. Here, we determine the cryoEM structure of a single protofilament of FtsZ from Klebsiella pneumoniae (KpFtsZ) in a polymerization-preferred conformation. We also develop a monobody (Mb) that binds to KpFtsZ and FtsZ from Escherichia coli without affecting their GTPase activity. Crystal structures of the FtsZ-Mb complexes reveal the Mb binding mode, while addition of Mb in vivo inhibits cell division. A cryoEM structure of a double-helical tube of KpFtsZ-Mb at 2.7 Å resolution shows two parallel protofilaments. Our present study highlights the physiological roles of the conformational changes of FtsZ in treadmilling that regulate cell division.