Protein Domains and Signaling Interactions
Signaling specificity in cells is built largely from modular protein-interaction domains — compact, independently folding units such as SH2, SH3, PTB, PH, and PDZ domains — that recognize particular sequence motifs, post-translational modifications, or membrane lipids. By combining these domains, proteins are wired into defined signaling networks.
Definition
A signaling interaction domain is a modular, independently folding protein region that mediates a specific binding interaction — recognizing a defined peptide motif, a post-translational modification, or a membrane lipid — and thereby links signaling proteins into pathways.
Scope
This topic covers the concept of modular interaction domains, the principal domain families and what each recognizes, and how domain combinations create the connectivity and specificity of signaling pathways, with receptor tyrosine kinase signaling as a worked example. It is mechanistic reference material.
Core questions
- How do modular domains generate the specificity of signal transduction?
- What kinds of marks do interaction domains recognize?
- How does combining domains in one protein wire a signaling network?
Key concepts
- Modular interaction domains
- SH2 domains (phosphotyrosine recognition)
- SH3 domains (proline-rich motif recognition)
- PTB domains
- PH domains (membrane phosphoinositide binding)
- PDZ domains (C-terminal motif recognition)
- Combinatorial domain assembly and network connectivity
Mechanisms
Many signaling proteins are mosaics of small interaction domains that each bind a defined target, so that the overall protein behaves as a programmable connector. SH2 domains recognize specific phosphotyrosine-containing motifs and so couple signaling to tyrosine phosphorylation; SH3 domains bind proline-rich sequences; PTB domains read phosphotyrosine and adjacent residues; PH domains bind particular membrane phosphoinositides to localize proteins to membranes; and PDZ domains recognize the carboxy-terminal motifs of partner proteins (Pawson & Nash, 2003). Because these domains read post-translational modifications, an enzyme that adds or removes a modification can rapidly rewire which partners assemble (Seet et al., 2006). Receptor tyrosine kinases illustrate the logic: ligand-induced autophosphorylation creates phosphotyrosine docking sites that recruit SH2- and PTB-domain proteins, nucleating a downstream signaling complex (Schlessinger, 2000; Lemmon & Schlessinger, 2010).
Clinical relevance
Interaction domains define how growth-factor and other signals are propagated, and mutations or aberrant phosphorylation that alter domain-mediated binding are studied in disease contexts including cancer (Lemmon & Schlessinger, 2010). The entry describes these binding principles as reference knowledge, not as clinical guidance.
Evidence & guidelines
The topic draws on cell-signaling and structural-biology reviews of modular interaction domains (Pawson & Nash, 2003; Seet et al., 2006; Schlessinger, 2000; Lemmon & Schlessinger, 2010) rather than clinical guidelines.
History
The modular view of signaling proteins emerged in the late 1980s and 1990s with the recognition that SH2 and SH3 domains are transferable binding modules, leading to a general model in which signaling networks are assembled from combinations of interaction domains (Pawson & Nash, 2003).
Key figures
- Tony Pawson
- Joseph Schlessinger
- Mark Lemmon
- Ivan Dikic
Related topics
Seminal works
- pawson-2003
- schlessinger-2000
- seet-2006
Frequently asked questions
- What does an SH2 domain recognize?
- An SH2 domain binds short peptide motifs that contain a phosphorylated tyrosine, which is how it couples signaling to tyrosine phosphorylation events.
- Why are interaction domains described as modular?
- Each domain folds and functions independently, so it can be combined with other domains in many proteins, allowing cells to build diverse signaling connections from a limited set of recognition units.