A New Membrane Protein Sbg1 Links the Contractile Ring Apparatus and Septum Synthesis Machinery in Fission Yeast

摘要

Cytokinesis in many organisms requires a plasma membrane anchored actomyosin ring, whose contraction facilitates cell division. In yeast and fungi, actomyosin ring constriction is also coordinated with division septum assembly. How the actomyosin ring interacts with the plasma membrane and the plasma membrane-localized septum synthesizing machinery remains poorly understood. In Schizosaccharomyces pombe , an attractive model organism to study cytokinesis, the β-1,3-glucan synthase Cps1p / Bgs1p, an integral membrane protein, localizes to the plasma membrane overlying the actomyosin ring and is required for primary septum synthesis. Through a high-dosage suppressor screen we identified an essential gene, sbg1 ~( + )( s uppressor of b eta g lucan s ynthase 1), which suppressed the colony formation defect of Bgs1-defective cps1-191 mutant at higher temperatures. Sbg1p, an integral membrane protein, localizes to the cell ends and to the division site. Sbg1p and Bgs1p physically interact and are dependent on each other to localize to the division site. Loss of Sbg1p results in an unstable actomyosin ring that unravels and slides, leading to an inability to deposit a single contiguous division septum and an important reduction of the β-1,3-glucan proportion in the cell wall, coincident with that observed in the cps1-191 mutant. Sbg1p shows genetic and / or physical interaction with Rga7p, Imp2p, Cdc15p, and Pxl1p, proteins known to be required for actomyosin ring integrity and efficient septum synthesis. This study establishes Sbg1p as a key member of a group of proteins that link the plasma membrane, the actomyosin ring, and the division septum assembly machinery in fission yeast. Author Summary Cell division in many organisms requires the function of an actomyosin ring, an apparatus that resembles the force generating machinery in the muscle. This ring apparatus is attached to the cell periphery (cell membranes) such that when it contracts, it brings the cell periphery together with it, leading to cell division. How the actomyosin ring is attached to the cell membrane at the division site is unknown. In this manuscript, we identify and describe Sbg1, a protein that links the actomyosin ring and the cell membranes since Sbg1 has a sequence that allows it to be inserted into the cell membrane. Sbg1 specifically localizes to the cell division site and also cooperates with a cell wall biosynthetic enzyme Bgs1 to achieve cell division. Consistently, in the absence of Sbg1, cells fail to divide leading to lethality. Sbg1 interacts with a number of cell division proteins, such as Cdc15, Rga7, Imp2, and Pxl1, to achieve its function as a bridge between the cell membrane and the actomyosin ring. Our work identifies a direct molecular link between the actomyosin ring and the cell membranes, explaining how ring contraction leads to inward movement of the cell periphery.