Brain tumours and neurofibromatosis Flashcards
Epidemiology of brain tumours:
2nd most common paediatric cancer
In adults - usually supratentorial, in children - posterior fossa mainly.
Majority are gliomas (glial cell in origin): Astrocytomas (85%-90%), Oligodendroglioma (5%).
Astrocytoma most common - most malignant grade is called a Glioblastoma Multiforme.
Risk factors of primary brain tumour?
More common in affluent groups.
Ionising radiation, vinyl chloride, immunosuppression.
Family history of Neurofibromatosis, tuberous sclerosis, Von-Hippel-Lindau syndrome
Types of brain tumour?
1) Glioma - astrocytoma (most common + glioblastoma multiform is most malignant), oligodendroglioma arises from oligodendrocytes and grows slowly over several years, may present with seizures + IDH1 mutation positive.
2) Ependymoma - raising from ependymal cells lining ventricles and spinal cord.
3) Meningioma - most common in older men and women, benign and arises from arachnoid mater and may grow to a large size over years pushing into brain.
4) Neurofibroma - arises from Schwann cells
Tumours be it malignant of benign act as space-occupying lesions within the brain = raised ICP which can eventually result in coning (herniation of brain through foramen magnum leading to compressed brainstem).
Clinical presentation of tumours?
4 cardinal presenting symptoms:
1) Symptoms of raised ICP - headache (morning, cough/strain/bending, relieved by vomitting), drowsiness/ALOC, vomitting, papilloedema (swollen optic disc, retinal oedema, loss of crisp optic nerve head margins (take days)). Bradycardia, high BP.
2) Progressive neurological deficit: Depends on area of brain that is affected.
Frontal lobe - Broca’s dysphasia, motor dysfunction (hemiparesis), cognitive decline, personality change, planning.
Temporal lobe - amnesia (memory loss), Wernicke’s dysphasia
Parietal lobe - Hemisensory loss, reduction in 2-point discrimination, dysphasia, asterogenesis
Occipital lobe - Contralateral visual loss
Cerebellum - Dysdiochokinesia, dysmetria, ataxia, speech slurred, hypotonia, intention tremor, nystagmus, gait disturbance.
3) Epilepsy/seizure - More focal/partial seizures - with motor, sensory, and temporal lobe pattern with de ja vu, olfactory aura, and funny feeling in stomach before and during seizure.
4) Lethargy/tiredness due to compression of brainstem.
What are other examples of space-occupying lesions?
Aneurysm, hydrocephalus, abscess, haemorrhage
Diagnosis of primary brain tumour?
1) CT and MRI - MRI superior for posterior fossa lesions, determine size and location, high grade tumours have irregular edges and high growth rate.
2) Blood tests: FBC, U & E’s, LFT, B12 etc.
3) Biopsy - via skull burr-hole - to determine cancer grade and confirm.
4) LP - is contraindicated when there is any possibility of a mass lesion since withdrawing CSF may provoke immediate coning.
Treatment of a primary brain tumour?
1) Surgery to remove mass if possible
2) Radiotherapy if surgery is not possible
3) Chemotherapy for glioma - at same time as surgery and 1st 6 weeks post-op (Temozolomide). Not all tumours are sensitive as they have high MGMT - ensure MGMT is methylated before administering.
4) IV Dexamethasone - improves brain function and reduces oedema and inflammation of tumour
5) IV Carbamazepine - anti-convulsants
What are the commonest neoplasms to metastasise to CNS in order?
1) Non small cell lung (most common)
2) Small cell lung
3) Breast
4) Melanoma
5) Renal cell
6) GI (least common)
Treatment for secondary brain tumours?
1) Surgery if (<75 yrs)
2) Radiotherapy
3) Chemotherapy
4) Palliative
Neurofibromatosis aetiology + epidemiology?
Autosomal dominant condition causing lesions in skin, nervous system and skeleton.
NF1 - Von Recklinghausen’s disease - caused by gene mutation 17 affecting 1 in 4000.
NF2 - much rarer and caused by gene mutation 22 affecting 1 in 100,000, presenting with CNS tumours rather the skin lesions.
Difference between NF1 and NF2?
- NF1 presents in childhood, NF2 between 20-40yrs.
- 45% of NF2 presents with hearing problems such as deafness/tinnitus +/- loss of balance/facial weakness.
- NF1 has early onset of cafe-au-lait spots but fewer spots in NF2 (<6).
Other conditions with cafe-au-lait spots?
1) Hereditary non-polyposis cancer of the colon.
2) DNA repair syndromes
3) McCune-Albright syndrome
NF1 criteria of diagnosis?
> 2 of the following:
1) >6 cafe-au-lait spots - flat, coffee-coloured patches of skin seen in first year of life increasing in number and size with age.
2) >2 neurofibromas - Dermal - small skin nodules after puberty. Nodular - Subcutaneous, firm nodules that can cause parasthesia if compressed.
3) >2 Lisch nodules - nodules of the iris only seen with slit lamp.
4) Pheochromocytoma - tumour of the Adrenal gland causing increased adrenaline/noradrenaline - high BP and sweating
5) First degree relative with NF1
6) Freckling of axilla, groin, sub-mammary in women, neck base present by age 10.
NF2 criteria of diagnosis
1 of:
1) Bilateral vestibular Schwannoma (CN8) - acoustic neuroma with hearing loss, vertigo, tinnitus
OR
2) 1st degrees relative with NF2 AND either unilateral vestibular Schwannoma or >1 neurofibroma/glioma
Treatment of neurofibromatosis?
1) Neurosurgery to remove tumours
2) Radio/Chemo if location or surgery is difficult
3) Surveillance
