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Extracellular polyphosphate signals through Ras and Akt to prime Dictyostelium discoideum cells for development
Author(s) -
Patrick M. Suess,
Jacob Basil Watson,
Wensheng Chen,
Richard H. Gomer
Publication year - 2017
Publication title -
journal of cell science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.384
H-Index - 278
eISSN - 1477-9137
pISSN - 0021-9533
DOI - 10.1242/jcs.203372
Subject(s) - polyphosphate , dictyostelium discoideum , biology , microbiology and biotechnology , cytokinesis , extracellular , protein kinase b , actin , dictyostelium , cytoskeleton , signal transduction , biochemistry , cell , cell division , phosphate , gene
Linear chains of five to hundreds of phosphates called polyphosphate are found in organisms ranging from bacteria to humans, but their function is poorly understood. In Dictyostelium, polyphosphate is used as a secreted signal that inhibits cytokinesis in an autocrine negative feedback loop. To elucidate how cells respond to this unusual signal, we did proteomic analysis of cells treated with physiological levels of polyphosphate and observed that polyphosphate causes cells to decrease levels of actin cytoskeleton proteins, possibly explaining how polyphosphate inhibits cytokinesis. Polyphosphate also causes proteasome protein levels to decrease, and in both Dictyostelium and human leukemia cells, decreases proteasome activity and cell proliferation. Polyphosphate also induces Dictyostelium cells to begin development by increasing expression of the cell-cell adhesion molecule CsA and causing aggregation, and this effect, as well as the inhibition of proteasome activity, is mediated by Ras and Akt. Surprisingly, Ras and Akt do not affect the ability of polyphosphate to inhibit proliferation, suggesting that a branching pathway mediates the effects of polyphosphate, with one branch affecting proliferation, and the other branch affecting development.

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