Affiliation:
1. Department of Anatomy and Cell Biology, Columbia University, New York, New York 10032
2. Department of Biology, Allegheny College, Meadville, Pennsylvania 16335
3. Department of Biology, Amherst College, Amherst, Massachusetts 01002
Abstract
ABSTRACT
Dictyostelium discoideum
amoebae with an altered
fbxA
gene, which is thought to encode a component of an SCF E3 ubiquitin ligase, have defective regulation of cell type proportionality. In chimeras with wild-type cells, the mutant amoebae form mainly spores, leaving the construction of stalks to wild-type cells. To examine the role of
fbxA
and regulated proteolysis, we have recovered the promoter of
fbxA
and shown that it is expressed in a pattern resembling that of a prestalk-specific gene until late in development, when it is also expressed in developing spore cells. Because
fbxA
cells are developmentally deficient in pure culture, we were able to select suppressor mutations that promote sporulation of the original mutant. One suppressor mutation resides within the gene
regA
, which encodes a cyclic AMP (cAMP) phosphodiesterase linked to an activating response regulator domain. In another suppressor, there has been a disruption of
dhkA
, a gene encoding a two-component histidine kinase known to influence
Dictyostelium
development. RegA appears precociously and in greater amounts in the
fbxA
mutant than in the wild type, but in an
fbx
A/
dhk
A double mutant, RegA is restored to wild-type levels. Because the basis of
regA
suppression might involve alterations in cAMP levels during development, the concentrations of cAMP in all strains were determined. The levels of cAMP are relatively constant during multicellular development in all strains except the
dhkA
mutant, in which it is reduced at least sixfold. The level of cAMP in the double mutant
dhkA/fbxA
is relatively normal. The levels of cAMP in the various mutants do not correlate with spore formation, as would be expected on the basis of our present understanding of the signaling pathway leading to the induction of spores. Altered amounts of RegA and cAMP early in the development of the mutants suggest that both
fbxA
and
dhkA
genes act earlier than previously thought.
Publisher
American Society for Microbiology
Subject
Molecular Biology,General Medicine,Microbiology
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