A glioma is a primary brain tumor that arises from glial cells — astrocytes, oligodendrocytes, or ependymal cells — within the central nervous system. Gliomas account for about 80% of malignant primary brain tumors. The 2021 WHO classification groups them by molecular markers including IDH mutation, 1p/19q codeletion, and others.

Is glioma always cancer?

Most adult diffuse gliomas (astrocytoma, oligodendroglioma, glioblastoma) are malignant (WHO grade 2-4). Pilocytic astrocytoma (WHO grade 1) is considered benign and is often curable by surgery. The 2021 WHO classification uses molecular markers in addition to grade to refine prognosis and treatment.

What is glioblastoma?

Glioblastoma (IDH-wildtype, WHO grade 4) is the most common and most aggressive adult diffuse glioma. Median overall survival with the Stupp protocol (surgery, radiotherapy, temozolomide) is 14-18 months; adding Tumor Treating Fields extends it to 20-21 months. MGMT-methylated tumors have the best outcomes.

What are the first signs of a brain tumor?

Common early signs include new or progressively worsening headache (often worse in the morning), first-ever seizure in an adult, new focal weakness or numbness, language or memory changes, personality changes, visual disturbance, and persistent nausea or vomiting. Any of these in an adult warrants brain MRI with contrast.

How is glioma diagnosed?

Diagnosis begins with brain MRI with and without gadolinium contrast. Tissue obtained at surgery or stereotactic biopsy is examined for histology and molecular markers (IDH, 1p/19q, MGMT, CDKN2A/B, EGFR, TERT, and others). The 2021 WHO classification integrates histology and molecular data into a single diagnosis.

How is glioblastoma treated?

Standard treatment is maximal safe surgical resection followed by 60 Gy of focal radiotherapy with concurrent daily temozolomide, then 6 cycles of adjuvant temozolomide every 28 days. Tumor Treating Fields added to adjuvant therapy extends survival. Recurrent disease may be treated with re-resection, bevacizumab, lomustine, regorafenib, or clinical trial.

What is the survival rate for glioma?

Survival varies dramatically by type. Glioblastoma 5-year survival is approximately 7%. IDH-mutant grade 4 astrocytoma 5-year survival is 30-50%. Grade 2-3 oligodendroglioma with 1p/19q codeletion has median survival of 14-18 years. Pilocytic astrocytoma has 10-year survival over 90% with complete resection.

What are IDH mutations and why do they matter?

IDH1 and IDH2 mutations occur in most lower-grade adult diffuse gliomas and predict longer survival than IDH-wildtype glioblastoma. They also identify candidates for IDH-inhibitor therapy. The 2021 WHO classification uses IDH status to define glioma type and direct treatment.

What is the MGMT methylation status?

MGMT promoter methylation silences a DNA-repair enzyme that protects glioma cells from alkylating chemotherapy. Methylated tumors respond better to temozolomide; in glioblastoma, methylated patients have median survival over 21 months vs. about 13 months for unmethylated, and methylation guides treatment decisions especially in older adults.

Vorasidenib is an oral IDH1/IDH2 inhibitor that crosses the blood-brain barrier and suppresses 2-hydroxyglutarate production in IDH-mutant glioma cells. The phase 3 INDIGO trial showed median progression-free survival of 27.7 vs 11.1 months with placebo in residual IDH-mutant grade 2 glioma after surgery. FDA approved in 2024.

What are Tumor Treating Fields?

Tumor Treating Fields (Optune) deliver alternating electric fields through scalp-mounted transducer arrays worn at least 18 hours per day. In the EF-14 trial, adding TTFields to adjuvant temozolomide in newly diagnosed glioblastoma increased median survival from 16.0 to 20.9 months and 5-year survival from 5% to 13%.

Are brain tumors caused by cell phones?

No consistent link has been established between mobile phone use and glioma in large prospective cohorts, including the Million Women Study and recent pooled analyses. Older case-control data showed weak associations that were not replicated in higher-quality studies. Therapeutic ionizing radiation is the established environmental risk factor.

Can gliomas be inherited?

Most gliomas are sporadic. Less than 5% occur in hereditary syndromes such as neurofibromatosis type 1, Li-Fraumeni syndrome (TP53), Lynch syndrome, and constitutional mismatch-repair deficiency. A first-degree relative with brain tumor about doubles personal risk, but absolute risk remains low.

What is awake craniotomy?

Awake craniotomy is a surgical technique in which the patient is woken during tumor resection to allow real-time mapping of motor, language, and cognitive function. It reduces permanent neurological deficit by 50-70% in eloquent-area tumors while allowing maximal safe resection. Pain is controlled with local anesthesia.

Do all gliomas need surgery?

Maximal safe resection is the goal for most gliomas because it provides definitive diagnosis and extends survival. Deep, brainstem, or eloquent-area tumors that cannot be safely resected are biopsied stereotactically to obtain tissue for molecular analysis before non-surgical treatment. Watch-and-wait is used for some asymptomatic low-grade tumors.

What is the difference between glioma and meningioma?

Glioma arises from glial cells within brain parenchyma and is infiltrative. Meningioma arises from arachnoid cells in the meninges and is typically a well-circumscribed, dural-based mass. Meningiomas are usually WHO grade 1 with excellent prognosis; most gliomas are malignant with more complex treatment.

Can a glioma be cured?

Pilocytic astrocytoma (WHO grade 1) can often be cured by complete surgical resection. Adult diffuse gliomas, including all IDH-mutant astrocytomas, oligodendrogliomas, and glioblastomas, are not curable with current therapy and ultimately recur, but treatment can extend survival substantially and preserve function.

What happens at glioma recurrence?

Options at recurrence include re-resection, repeat focal radiotherapy or stereotactic radiosurgery, second-line chemotherapy (lomustine, regorafenib, bevacizumab), targeted therapy if a tractable alteration is present, and clinical trial enrollment. Decisions are made by a multidisciplinary tumor board.

Do gliomas cause seizures?

Yes. Tumor-related seizures occur in 40-60% of low-grade gliomas and 20-30% of glioblastomas. Levetiracetam is preferred for prophylaxis and treatment because of minimal drug interactions. Maximal tumor resection improves seizure control. Routine antiepileptic prophylaxis in seizure-free patients is not recommended.

Can someone drive after a glioma diagnosis?

Driving restrictions apply after a seizure or after craniotomy, with seizure-free intervals (often 6-12 months) required by local law. Restrictions also depend on visual field, cognition, and motor function. Patients should consult their treatment team and review local driver-licensing regulations.

How often is follow-up imaging needed?

Follow-up MRI is typically every 2-3 months in the first 1-2 years after treatment, then every 4-6 months. Frequency is adjusted based on tumor grade, molecular markers, and clinical course. Imaging at first sign of new symptoms is essential to distinguish progression from treatment-related changes such as pseudoprogression.

Neurosurgerycritical

Brain Tumor (Glioma).Care & specialists in Mexico

In Mexico, brain Tumor (Glioma) is managed by neurosurgerys. Glioma is a group of primary brain tumors that arise from glial cells (astrocytes, oligodendrocytes, ependymal cells) and accounts for approximately 27% of all primary brain tumors and 80% of malignant primary brain tumors. The age-adjusted annual incidence is roughly 6 per 100,000 in the United States, with a slight male predominance and peak between ages 55 and 70.

Reviewed by AIHealz Medical Editorial Board · NeurosurgeryLast reviewed May 13, 2026

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What it is

Gliomas (ICD-10: C71.x for malignant neoplasm of brain; D33.x for benign; D43.x for uncertain behavior) are primary central nervous system tumors arising from cells of glial lineage — astrocytes, oligodendrocytes, and ependymal cells. The 2021 WHO Classification of CNS Tumors (CNS5) integrates histology with molecular features into the diagnosis, replacing the older purely-histologic system. Adult-type diffuse gliomas now include three families: astrocytoma IDH-mutant (grades 2, 3, 4); oligodendroglioma IDH-mutant and 1p/19q-codeleted (grades 2, 3); and glioblastoma IDH-wildtype (grade 4). Pediatric-type diffuse gliomas (low-grade and high-grade), circumscribed astrocytic gliomas (pilocytic astrocytoma, pleomorphic xanthoastrocytoma, subependymal giant cell astrocytoma), glioneuronal and neuronal tumors, and ependymal tumors form additional families.

Types and stages

Glioblastoma, IDH-wildtype (WHO grade 4)The most common and aggressive adult diffuse glioma. Defined by IDH-wildtype status with at least one of: TERT promoter mutation, EGFR amplification, or +7/-10 chromosome pattern, or by histological glioblastoma features. Median overall survival 14-18 months with optimal therapy; MGMT-methylated tumors have better temozolomide response and longer survival.

Astrocytoma, IDH-mutant (WHO grade 2, 3, 4)Diffuse astrocytic glioma with IDH1 R132H or IDH2 mutation. Grade is determined by histology and CDKN2A/B homozygous deletion (grade 4 if present). Median survival 6-10 years for grade 2-3 and 4-5 years for grade 4 IDH-mutant astrocytoma — substantially better than IDH-wildtype glioblastoma.

Oligodendroglioma, IDH-mutant and 1p/19q codeleted (WHO grade 2, 3)Defined by IDH mutation plus whole-arm codeletion of chromosomes 1p and 19q. Most chemo- and radiotherapy-responsive adult diffuse glioma; median overall survival 14-18 years with combined RT and PCV chemotherapy in RTOG 9802 and 9402 trials.

Pediatric-type high-grade glioma (diffuse midline glioma H3 K27-altered; diffuse hemispheric glioma H3 G34-mutant)Aggressive pediatric and young-adult tumors driven by H3 histone mutations. Diffuse midline glioma of the pons (formerly DIPG) carries median survival under 1 year. H3 G34-mutant tumors arise in cerebral hemispheres of older children and young adults.

Pilocytic astrocytoma (WHO grade 1)Circumscribed, often cystic tumor most common in children and young adults, typically in cerebellum, optic pathway, or hypothalamus. BRAF fusion or mutation in many. Surgical cure rates over 90% when complete resection is feasible; 10-year overall survival above 90%.

Ependymoma (supratentorial, posterior fossa, spinal)Tumor of ependymal cells of ventricles and central canal. Posterior fossa ependymoma in children is the most common form; supratentorial ZFTA-fused ependymoma has worse prognosis. Treatment combines maximal safe resection with focal radiotherapy.

Living with Brain Tumor (Glioma)

Timeline

Hospital recovery after craniotomy: 3-7 days. Initial functional recovery: 4-8 weeks with neurorehabilitation if needed. Concurrent chemoradiation: 6 weeks of daily treatment followed by 4-week break. Adjuvant temozolomide cycles: 6 cycles over 6 months. Tumor Treating Fields: continued at least 18 hours/day for months to years until progression. Surveillance MRI every 2-3 months in the first 1-2 years, then every 4-6 months.

Lifestyle

01Maintain seizure precautions during active disease: driving restrictions per local law, avoidance of unsupervised swimming, height work, and operation of heavy machinery.
02Follow medication schedules strictly for temozolomide, anti-epileptic agents, and corticosteroids; missed doses can have significant consequences.
03Monitor and report new or worsening symptoms (headache, weakness, seizure, language change) promptly between scheduled visits.
04Use nutrition and exercise programs to counter steroid-induced weight gain, muscle loss, and bone-density loss.
05Engage early with palliative care and supportive services regardless of prognosis — improves quality of life and may extend survival.
06Maintain social and cognitive engagement during and after treatment to support recovery and quality of life.

Daily management

01Take temozolomide and other oral oncology drugs at the same time each day, on an empty stomach with anti-emetic premedication during induction cycles.
02Monitor and record temperature, headache severity, seizures, and any new neurological symptoms.
03Wear Tumor Treating Fields transducer arrays at least 18 hours per day if prescribed.
04Apply moisturizers and protect scalp skin during radiotherapy and TTFields use.
05Use a written symptom diary to share with the neuro-oncology team at follow-up visits.
06Maintain a current medication list including supplements; alert the team to any new prescription or over-the-counter product.

Exercise

Aerobic and resistance exercise is recommended during and after treatment when safely tolerated. Even 20-30 minutes of walking 3-5 times per week reduces fatigue, improves mood, and supports cognitive function. Avoid contact sports and activities with fall risk while seizures are uncontrolled or anticoagulation is needed. Coordinate with neurorehabilitation for tailored programs after neurological deficit.

Brain Tumor (Glioma).Care & specialists in Mexico

What it is

How you might notice it

How it’s diagnosed

Treatment & cost

Causes & risk factors

Living with it

When to seek help

Related conditions

Easily confused with

Often appears alongside

Types and stages

Living with Brain Tumor (Glioma)

Complementary approaches

Patient support resources

Frequently asked

Sources & references

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