Phosphoproteomic Profiling Reveals Overlapping And Distinct Signaling Pathways In Dictyostelium Discoideum In Response To Two Different Chemorepellents
Document Type
Article
Publication Date
1-1-2026
School
Biological, Environmental, and Earth Sciences
Abstract
Chemorepulsion mechanisms for eukaryotic cells are poorly understood. We performed proteomics and phosphoproteomics to elucidate how Dictyostelium discoideum responds to its two endogenous chemorepellent signals, the protein AprA and inorganic polyphosphate (polyP). AprA and polyP affected levels of more than 200 proteins, with an overlap of both upregulating 25 proteins and downregulating two proteins. Two proteins were upregulated by AprA but downregulated by polyP, while two others showed the opposite trend. Surprisingly, many of the AprA- and polyP-regulated proteins are associated with RNA metabolism and ribosomes. AprA increased phosphorylation of 15 proteins and decreased phosphorylation of 36 proteins. PolyP increased phosphorylation of 12 proteins and decreased phosphorylation of 12 proteins. As expected, the two chemorepellents affected phosphorylation of signal transduction/ motility proteins, but unexpectedly affected phosphorylation of RNA-associated proteins. Both AprA and polyP decreased phosphorylation of five proteins including the Ras-interacting protein RipA and guanine nucleotide exchange factors (GEFs) such as the RacGEF GxcT. Mutants lacking RipA or GxcT were unresponsive to both AprA and polyP chemorepulsion. Together, this work supports the idea that rather than activating the same chemorepulsion mechanism, AprA and polyP activate only partially overlapping chemorepulsion mechanisms, and identifies two new components that are used by both chemorepellents.
Publication Title
Cells
Volume
15
Issue
1
Recommended Citation
Uddin, S.,
Rijal, R.,
Pilling, D.,
Gomer, R.
(2026). Phosphoproteomic Profiling Reveals Overlapping And Distinct Signaling Pathways In Dictyostelium Discoideum In Response To Two Different Chemorepellents. Cells, 15(1).
Available at: https://aquila.usm.edu/fac_pubs/22010
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