
Emerging evidence indicates that complex spatial gradients and (micro)domains of signalling activities arise from distinct cellular localization of opposing enzymes, such as a kinase and phosphatase, in signal transduction cascades. Often, an interacting, active form of a target protein has a lower diffusivity than an inactive form, and this leads to spatial gradients of the protein abundance in the cytoplasm. A spatially distributed signalling cascade can create step‐like activation profiles, which decay at successive distances from the cell surface, assigning digital positional information to different regions in the cell. Feedback and feedforward network motifs control activity patterns, allowing signalling networks to serve as cellular devices for spatial computations.
Feedback, Physiological, MAP Kinase Signaling System, Protein modification cycle, Spatiotemporal dynamic, Cell Polarity, Biological Transport, spatiotemporal dynamics, Signal transduction, Phosphoproteins, spatial gradients, protein modification cycle, Spatial gradient, Protein Processing, Post-Translational, signal transduction, Cell Size
Feedback, Physiological, MAP Kinase Signaling System, Protein modification cycle, Spatiotemporal dynamic, Cell Polarity, Biological Transport, spatiotemporal dynamics, Signal transduction, Phosphoproteins, spatial gradients, protein modification cycle, Spatial gradient, Protein Processing, Post-Translational, signal transduction, Cell Size
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