Myosin concentration underlies cell size–dependent scalability of actomyosin ring constriction

Author:

Calvert Meredith E.K.12,Wright Graham D.3,Leong Fong Yew4,Chiam Keng-Hwee45,Chen Yinxiao1,Jedd Gregory15,Balasubramanian Mohan K.1255

Affiliation:

1. Temasek Life Sciences Laboratory, The National University of Singapore, Singapore 117604

2. Marine Biological Laboratory, Woods Hole, MA 02543

3. Institute of Medical Biology, A*STAR, Immunos, Singapore 138648

4. Institute of High Performance Computing, A*STAR, Singapore 138632

5. Mechanobiology Institute and Department of Biological Sciences, The National University of Singapore, Singapore 117543

Abstract

In eukaryotes, cytokinesis is accomplished by an actomyosin-based contractile ring. Although in Caenorhabditis elegans embryos larger cells divide at a faster rate than smaller cells, it remains unknown whether a similar mode of scalability operates in other cells. We investigated cytokinesis in the filamentous fungus Neurospora crassa, which exhibits a wide range of hyphal circumferences. We found that N. crassa cells divide using an actomyosin ring and larger rings constricted faster than smaller rings. However, unlike in C. elegans, the total amount of myosin remained constant throughout constriction, and there was a size-dependent increase in the starting concentration of myosin in the ring. We predict that the increased number of ring-associated myosin motors in larger rings leads to the increased constriction rate. Accordingly, reduction or inhibition of ring-associated myosin slows down the rate of constriction. Because the mechanical characteristics of contractile rings are conserved, we predict that these findings will be relevant to actomyosin ring constriction in other cell types.

Publisher

Rockefeller University Press

Subject

Cell Biology

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