Glioblastoma Genome [Neurosurgery Wiki]

glioblastoma_genome

A complex and heterogeneous genomic profile characterizes glioblastoma (GBM).

TP53 — Tumor suppressor gene; commonly mutated.
EGFR — Often amplified or mutated (e.g., *EGFRvIII* variant).
PTEN — Mutations/deletions → PI3K/AKT pathway activation.
IDH1/IDH2 — Mutated in secondary GBM, better prognosis.
TERT promoter — Mutated in primary GBM → ↑ telomerase.
NF1 — Inactivation seen in mesenchymal subtype.
PIK3CA / PIK3R1 — Activates PI3K pathway.

+Chromosome 7 / -Chromosome 10 — Hallmark alteration.
CDKN2A/B deletion — Affects p16INK4a and p14ARF (cell cycle).
MDM2 amplification — Inhibits p53 function.

MGMT promoter methylation — Increases sensitivity to temozolomide.
G-CIMP phenotype — IDH1-related, associated with better survival.

EGFR amplification
CDKN2A deletion
No TP53 mutation

NF1 deletion/mutation
High expression of CHI3L1, MET

IDH1 mutation
PDGFRA amplification
TP53 mutation

Expression of neuron-specific genes (e.g., NEFL, GABRA1)
*Note: classification debated*

RTK/RAS/PI3K Pathway
- EGFR, PDGFRA, PIK3CA, NF1
TP53 Pathway
- TP53, MDM2
RB Pathway
- CDKN2A/B, RB1

Gene / Marker	Alteration Type	Clinical Implication
TP53	Mutation	Loss of cell cycle control
EGFR	Amplification / EGFRvIII	Aggressive phenotype
PTEN	Deletion/mutation	↑ PI3K/AKT signaling
IDH1/2	Mutation	Secondary GBM, better prognosis
MGMT	Promoter methylation	Better response to TMZ
TERT promoter	Mutation	Poor prognosis
CDKN2A/B	Homozygous deletion	Cell cycle deregulation
NF1	Mutation	Mesenchymal subtype driver

The Cancer Genome Atlas Research Network. (2008). Comprehensive genomic characterization defines human glioblastoma genes and core pathways.
Brennan et al., Cell, 2013.
Verhaak et al., Cancer Cell, 2010.

glioblastoma_genome.txt
Last modified: 2025/04/30 22:03
by administrador