CD226 | QF-Pro Glossary

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Definition

CD226 (DNAM-1) is an activating receptor on T cells and NK cells that binds CD155 (and CD112). CD226 promotes cytotoxicity and cytokine production. Critically, inhibitory TIGIT competes for the same ligand with higher affinity. The CD226/TIGIT balance determines net signaling outcome–tumors shift this balance toward TIGIT-mediated suppression by upregulating CD155.

Activating

Promotes T/NK cell function

Binds CD155

Same ligand as TIGIT

Competes with TIGIT

Lower affinity loses

Balance Matters

Determines immune outcome

The CD226-TIGIT Axis

CD226 and TIGIT represent a classic activating-inhibitory receptor pair, analogous to CD28/CTLA-4. Both bind CD155Loading..., but with opposite functional outcomes. TIGIT has higher affinity, so when CD155 is abundant (as in tumors), TIGIT-mediated inhibition dominates.

This competition explains why simply measuring CD155 or TIGIT expression may be insufficient–the functional outcome depends on which receptor is engaged. FRET-based measurement could directly assess this.

Simplified

Competing Receptors: CD226 and TIGIT both bind CD155, but have opposite effects. CD226 activates immune cells; TIGIT suppresses them.

The Balance Matters: Whether immune cells attack or stand down depends partly on which receptor "wins" the competition for CD155 binding.

Therapeutic Implications

Anti-TIGIT/CD155Loading...|TIGIT}} antibodies aim to block the inhibitory signal, shifting the balance toward CD226-mediated activation. Clinical trials combining anti-TIGIT with anti-PD-1 are ongoing.

CD226 itself can be downregulated on exhausted T cells, contributing to dysfunction. Measuring the CD226/TIGIT ratio and their respective engagement states could predict which patients will benefit from TIGIT blockade.

Simplified

Drug Development: Anti-TIGIT drugs aim to block the suppressive interaction, allowing CD226 to dominate.

Patient Selection: Measuring which interaction predominates could potentially identify patients most likely to benefit from TIGIT-targeted therapy.

QF-Pro Application

Exploratory

Theoretical Application: CD226 competes with TIGIT for CD155 binding, creating an immune activation/suppression balance. QF-Pro could potentially measure both CD226/CD155 and TIGIT/CD155 interactions, providing functional insight into net immune regulatory state.

Status: Theoretical application. Dual-target measurement could provide unique biological insight.

Note: This represents a theoretical application based on validated QF-Pro principles. Clinical validation studies are pending. See QF-Pro Applications for validated targets.

Simplified

Future potential: CD226 is the "activating" receptor competing with TIGIT. Measuring both interactions simultaneously could reveal the net immune regulatory state in individual tumors.

Clinical Relevance

Anti-TIGIT/CD155Loading...|TIGIT}} rationale: Blocking TIGIT tips balance toward CD226 activation
Biomarker potential: CD226 expression/engagement may predict response
Exhaustion marker: CD226 downregulation indicates T cell dysfunction
Combination therapy: TIGIT + PD-1 blockade in clinical trials

Connected Terms

CD155 Category Cross-ref Related
TIGIT/CD155 Category Cross-ref Related
ICI Category Related
TiME Category Related
T Cell Exhaustion Related
QF-Pro Applications & Clinical Evidence Cross-ref
4-1BB/4-1BBL Category
CEACAM1 Category