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1 Howard Hughes Medical Institute and
2 Department of Biochemistry and Cell Biology, MS-140, Rice University, 6100 South Main Street, Houston, TX 77005-1892, USA
*Author for correspondence (e-mail: richard{at}bioc.rice.edu)
Accepted 15 May 2002
Dictyostelium aggregation streams break up into groups of 103 to 2x104 cells. The cells sense the number of cells in a stream or group by the level of a secreted counting factor (CF). CF is a complex of at least 5 polypeptides. When the gene encoding countin (one of the CF polypeptides) was disrupted, the cells could not sense each others presence, resulting in non-breaking streams that coalesced into abnormally large groups. To understand the function of the components of CF, we have isolated cDNA sequences encoding a second component of CF, CF50. CF50 is 30% identical to lysozyme (but has very little lysozyme activity) and contains distinctive serine-glycine motifs. Transformants with a disrupted cf50 gene, like countin cells, form abnormally large groups. Addition of recombinant CF50 protein to developing cf50 cells rescues their phenotype by decreasing group size. Abnormalities seen in aggregating countin cells (such as high cell-cell adhesion and low motility) are also observed in the cf50 cells. Western blot analysis of conditioned medium sieve column fractions showed that the CF50 protein is present in the same fraction as the 450 kDa CF complex. In the absence of CF50, secreted countin is degraded, suggesting that one function of CF50 may be to protect countin from degradation. However, unlike countin cells, cf50 cells differentiate into an abnormally high percentage of cells expressing SP70 (a marker expressed in a subset of prespore cells), and this difference can be rescued by exposing cells to recombinant CF50. These observations indicate that unlike other known multisubunit factors, CF contains subunits with both overlapping and unique properties.
Key words: Counting factor, Cell population size, Dictyostelium discoideum
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