KRAS | QF-Pro Glossary

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Definition

KRAS is a small GTPase that acts as a molecular switch in growth factor signaling. KRAS mutations occur in ~25% of all cancers–pancreatic (~90%), colorectal (~40%), and lung (~25%). For decades, KRAS was considered 'undruggable' due to its smooth protein surface. KRAS G12C inhibitors (sotorasib, adagrasib) represent a breakthrough, exploiting the unique cysteine to lock KRAS in its inactive state.

~25%

Of all cancers

G12C Druggable

Sotorasib, adagrasib

Other Mutations

G12D, G12V still challenging

GTP/GDP Switch

Molecular on/off

The RAS Switch

KRAS cycles between active (GTP-bound) and inactive (GDP-bound) states. GTPase-activating proteins (GAPs) accelerate GTP hydrolysis; guanine nucleotide exchange factors (GEFs) promote GTP loading. Oncogenic mutations impair GTPase activity, locking KRAS in the active state.

Active KRAS engages effector proteins (RAF, PI3K) through protein-protein interactionsLoading..., driving downstream signaling cascades that promote proliferation and survival.

Simplified

What KRAS Does: KRAS is a molecular switch that cycles between "on" (GTP-bound) and "off" (GDP-bound). It transmits growth signals from receptors to downstream pathways.

When Mutated: Oncogenic KRAS mutations lock it in the "on" position, constantly signaling growth regardless of upstream signals.

Breaking the 'Undruggable' Barrier

KRAS's smooth surface and picomolar GTP affinity made traditional drug design impossible. The breakthrough came from recognizing that G12C creates a unique druggable pocket. Covalent inhibitors form irreversible bonds with the mutant cysteine, trapping KRAS in the inactive GDP-bound state.

Sotorasib (2021) and adagrasib (2022) are approved for KRAS G12C-mutant NSCLCLoading.... However, G12C represents only ~13% of KRAS mutations–G12D and G12V (more common) remain challenging targets.

Simplified

Historic Challenge: For decades, KRAS was considered "undruggable"—its smooth surface offered no pocket for drugs to bind.

Recent Breakthroughs: Sotorasib and adagrasib now target the G12C mutation. Other mutations are being targeted with newer approaches.

KRAS and Protein Interactions

KRAS function depends on effector protein interactions. Active KRAS binds RAF ('MAPK pathway) and PI3K ('Akt pathway) through specific protein-protein interactionLoading... domains. Different KRAS mutations may preferentially engage different effectors.

FRET-based measurement of KRAS-effector interactions could potentially assess pathway engagement and predict which downstream inhibitors might be effective in combination with KRAS inhibitors.

Simplified

Signaling Through Interactions: KRAS works by interacting with effector proteins (RAF, PI3K). Measuring these interactions could potentially assess pathway activity.

Downstream Readout: The validated Akt activation assay provides one window into KRAS pathway output, since PI3K/Akt is a major KRAS effector pathway.

Undruggable

KRAS considered impossible to target therapeutically

Mutation-Specific Drugs

G12C inhibitors exploit unique protein chemistry–more mutations coming

Clinical Applications

G12C testing: Required for KRAS G12C inhibitor eligibility in NSCLC
Approved drugs: Sotorasib, adagrasib for KRAS G12C NSCLC
Combinations: KRAS + SHP2, KRAS + checkpoint inhibitorsLoading... under investigation
Future targets: G12D inhibitors in clinical development

Connected Terms

BRAF Category Related Learning Path
EGFR Category Related Learning Path
NSCLC Cross-ref Related
HER2-HER3 Dimerization Category Learning Path
Colorectal Cancer Related
PI3K/Akt Pathway Related
Precision Medicine Related
PKB/Akt Category Learning Path