What are SMAD proteins?

SMADs are the intracellular messengers of the TGF-beta pathway: receptor-regulated SMADs are phosphorylated at the activated receptor, then partner with SMAD4 and move to the nucleus to regulate transcription.

Why is TGF-beta described as having opposite effects in cancer?

Its output depends on cellular context; in early stages it tends to restrain cell growth, whereas in advanced tumours it can promote invasion and immune evasion, so the same signal yields contrasting outcomes.

Transforming Growth Factor Beta Signaling

The transforming growth factor beta (TGF-beta) pathway converts an extracellular ligand into a nuclear transcriptional response through SMAD proteins. Ligand binding activates a pair of receptor serine/threonine kinases that phosphorylate receptor-regulated SMADs; these partner with a common SMAD, enter the nucleus, and regulate genes that control growth arrest, differentiation, and extracellular-matrix production.

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Definition

TGF-beta signalling is a pathway in which TGF-beta family ligands assemble type II and type I receptor serine/threonine kinases; the activated type I receptor phosphorylates receptor-regulated SMADs, which complex with the common-mediator SMAD4, translocate to the nucleus, and regulate transcription of target genes in cooperation with other factors.

Scope

The entry covers the TGF-beta ligand-receptor module, the SMAD activation and nuclear-transport cycle, the context-dependent gene programmes the pathway controls, and its dual roles in disease. It is reference material on mechanism, not clinical guidance.

Core questions

How does a serine/threonine-kinase receptor transmit a signal to the nucleus?
What is the role of SMAD proteins in carrying the signal?
How does the same pathway produce opposite outcomes in different contexts?
Why can TGF-beta act as both a tumour suppressor and a tumour promoter?

Key concepts

TGF-beta superfamily ligands
Type I and type II receptor serine/threonine kinases
Receptor-regulated SMADs (R-SMADs)
Common-mediator SMAD4
SMAD nuclear translocation and cofactors
Context-dependent transcriptional output
Growth inhibition and extracellular-matrix regulation

Mechanisms

A TGF-beta ligand brings together type II and type I receptor serine/threonine kinases; the constitutively active type II receptor phosphorylates and activates the type I receptor, which in turn phosphorylates receptor-regulated SMADs. These R-SMADs associate with the common-mediator SMAD4, accumulate in the nucleus, and bind DNA together with other transcription factors and cofactors to regulate target genes (Shi & Massague, 2003). The actual gene programme is highly context-dependent, shaped by the partner factors and chromatin state present in a given cell, which is why TGF-beta can produce growth arrest in one setting and very different responses in another (Massague, 2012). The pathway is regulated at multiple levels, including inhibitory SMADs that provide negative feedback.

Clinical relevance

TGF-beta signalling has a well-described dual role in cancer, restraining early tumour growth yet promoting invasion and immune evasion later, and it is a major driver of tissue fibrosis (Massague, 2012). This entry presents those associations as reference background and is not a basis for diagnostic or treatment decisions.

Evidence & guidelines

The pathway is established through biochemical, structural, and genetic studies synthesised in major reviews and is reference science rather than the subject of clinical guidelines. The cited reviews represent the consensus mechanism and its disease links.

History

TGF-beta was named for its early identification as a factor able to transform certain cells in culture, but its receptors were later found to be serine/threonine kinases, an unusual class for signalling receptors. Discovery of the SMAD proteins in the 1990s revealed how the receptors connect to the nucleus and established the receptor-to-SMAD-to-transcription framework used today.

Key figures

Joan Massague
Yigong Shi
Rik Derynck

Seminal works

shi-2003
massague-2012

Frequently asked questions

What are SMAD proteins?: SMADs are the intracellular messengers of the TGF-beta pathway: receptor-regulated SMADs are phosphorylated at the activated receptor, then partner with SMAD4 and move to the nucleus to regulate transcription.
Why is TGF-beta described as having opposite effects in cancer?: Its output depends on cellular context; in early stages it tends to restrain cell growth, whereas in advanced tumours it can promote invasion and immune evasion, so the same signal yields contrasting outcomes.