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INTRA CRANIAL SPACE OCCUPYING
LESIONS
DR.Bindu. K
BHMS,MD(HOM)
These are lesions which expand in volume to displace normal neural structures &
lead to increase in intra – cranial pressure.
PATHOLOGY :-
Symptoms are produced due to,
1. Irritation & destruction of brain tissue causing neurological phenomena,eg.
epilepsy, paralysis.
2. Raised intra cranial pressure:- The rate of increase of tension depend on the
nature of the lesion and its location. Posterior fossa lesions lead to more
rapid rise in tension than supratentorial lesions.
3. False localizing signs :-
• Neurological phenomena arising from the secondary effects of lesion like
herniation of neural tissue under the falx-cerebri or downward herniation
through tentorium cerebelli or foramen magnum, pressure effects on other parts
of brain develop.
• Countre – coup effect:- This is pressure effect caused on the side opposite to
the side of lesion when a space occupying lesion expands. The midline structures
such as brainstem may be pushed towards the opposite free margin of tentorium
cerebelli to give rise to compression of normal side also.
In addition to this , different lesions may produce symptoms specific to their
nature like fever in case of brain abscess, signs of meningeal irritation in
subarachnoid haemorrhage
Classification of intra cranial space occupying lesions :-
I. Congenital :- Dermoid, Epidermoid, Teratoma.
II. Traumatic :- Subdural & Extradural haematoma
III. Inflammatory :- Abscess, Tuberculoma, Syphilitic gumma,fungal Granulomas.
IV. Parasitic :- Cysticercosis, Hydratid cyst, Amebic abscess, Schistosoma
japonicum.
V. Neoplasms
a) Tumors arising from neural structures: Gliomas – astrocytoma, ependymoma,
oligodendroglioma, germinoma, medulloblastoma.
b) Tumors arising from appendages: Meningioma, schwannoma, chondroma, osteoma.
c) Pituitary lesions : Pituitary adenoma, Craniopharyngioma.
d) Vascular lesions : Angioma, Hemangioblastoma, Papilloma of choroid plexus.
e) Secondary neoplasms.
Clinical features :-
1. Persistent headache not due to any other detectable cause and
unresponsive to medication. This may be due to focal irritation, displacement of
pain sensitive structures or due to increased intra- cranial tension. If due to
increased intra- cranial tension headache develop rapidly over several minutes
persist for 20-40 minutes and subside quickly. May awaken the patient from sound
sleep 60-70 mts after retiring and also precipitated by coughing, sneezing,
vomiting etc.
2. Vomiting & visual loss :- projectile vomiting unassociated with nausea.
3. Papilledema in increased intra- cranial tension.
4. Recent onset behaviour changes.
5. Late onset seizures :- Any type of seizure occuring for the first time after
the age of 15 years should suggest the possibility of intra cranial space
occupying lesions. It is due to disruption of cortical circuits by tumours that
invade or compress cerebral cortex.
6. Sudden onset of neurological deficits like dementia, personality changes,
gait disorders etc.
INTRACRANIAL HAEMATOMAS
I. EXTRA DURAL HAEMATOMAS :-
Collection of blood between the dura & the skull due to injury to the middle
meningeal vein, middle meningeal artery, diploic vein, dural venous sinuses or
small vessels lying between dura and skull. Common site is temporal fossa.
Pathogenesis :-
Initial collection of blood in the extradural space causes stripping of the
dura from bone. Symptoms are produced when symptoms exceed 25 ml in volume.
Extent and location of haematomas are determined by the ease of stripping of the
dura, site of injury, its severity, and presence of depressed fractures of the
skull.
Clinical features :-
1. 1 – 2% persons suffering from head injury develop extra dural haematoma.
2. Uncommon in children below 3 yrs and in old age – adherance of dura
To the skull prevents its easy stripping.
3. Progressive deterioration of level of consciousness :- there may be a period
of immediate loss of consciousness, after that a period of apparent normalcy
with clear consciousness followed by deterioration of mental state.
4. Pupillary changes :- called Hutchinson’s pupillary reaction – pupil on the
side of lesion constricts initially then it dilates and as intra cranial tension
increases the opposite pupil also dilates.
Investigation :-
CT scan
MRI
Cerebral angiography.
II. SUBDURAL HAEMATOMAS :-
Collection of blood between the dura and the arachnoid. Usually
follow injuries which may be apparently trivial or even unnoticed. Common causes
are bleeding from superficial veins or venous sinuses. Anticoagulant treatment
predispose to intracranial bleeding and subdural haematoma. Usual sites are
frontal, anterior temporal,& parietal.
Pathology :-
Haematoma consists of fluid blood covered on inner and outer aspects by
layers of fibrin. Blood is defibrinated due to the constant pulsation of the
brain. High protein content of fluid makes it hyperosmotic. So it absorbs fluid
from the surrounding and enlarges leading to increase in intra cranial tension.
Clinical features :- Manifestation may be acute or chronic in nature.
Acute : Clinical features are similar to extra dural hematoma.
Chronic : Dementia, altered behaviour, psychiatric manifestations or
focal neurological deficits may develop.
In middle aged headache, contralateral hemiplegia, papilledema and in children
vomiting, restlessness. Irritability, refusal to feed, anaemia, seizures and
failure to thrive are common presenting symptoms.
Investigation :-
CT scan
MRI
Cerebral angiography.
NEOPLASMS OF BRAIN
About 50 % of intracranial tumors are primary neoplasms and the rest
secondary. Out of this 50 – 60 % of primary brain tumors are gliomas, 25% -
meningiomas, 10% - schwannoma and the remainder others.
Etiology:
1. Exposure to ionizing radiations is the only well documented enviornmental
risk factor.
2. A number of heriditary factors are associated with an increased risk of brain
tumours, eg. Neurofibromatosis type – I and type – II, Multiple endocrine
neoplasia type –I.
3. Genes also contribute to the development of brain tumours and other
malignancies. There are two classes of genes namely, tumour suppressor genes and
proto oncogenes. There is over – expression of proto oncogenes in brain tumours.
Clinical course of brain tumours :-
There are four stages of development of tumour.
Stage I : Initial period of silent growth.
Stage II : Stage of focal syndromes like epilepsy.
Stage III : Increased intracranial tension.
Stage IV : Brain displacement and false localizing signs.
PRIMARY NEOPLASMAS OF BRAIN :
I. Astrocytomas :
Derived from astrocytes. Common sites are cerebrum, cerebellum, thalamus, pons
and optic chiasma. Slow growing tumour. Most commonly used grading system is WHO
four tired grading system.
WHO grading,
Grade I – Least malignant with excellent prognosis after surgical excision, eg.
pilocytic astrocytoma.
Grade II - Astroblastoma
Grade III - Anaplastic astrocytoma
Grade IV - Glioblastoma multiforme – clinically aggressive
Astrocytomas occur in three forms namely, diffuse or infiltrating, solid and
cystic.
Prognosis :-
Poor prognosis in age over 65 years, poor functional status in grade III and
grade IV astrocytomas.
Low grade astrocytoma :- usually in children, spindle shaped cell (pilocytic
astrocytoma), occurs from cerebellum, well demarcated, cystic. Complete surgical
excision usually produces long term survival.
High grade astrocytoma :- seen in adults, usually supra – tentorial, no clearly
defined margins, infiltration to white matter and metastasis to spine through
CSF called drop metastasis occurs. Usually fatal and total surgical excision is
not possible.
Gliomatosis cerebri :-Rare form with diffuse infiltration of the brain by
malignant astrocytes without a focal enhancing mass.
Treatment :-whole brain radiation therapy in selected patients with
chemotherapy.
II. Oligodendrogliomas :-
Slow growing tumour compared to astrocytoma. They contain mixture of cells
with astrocytic and oligodendroglial features called mixed glioma. Usually
supratentorial. 50% of patients with 5 year survival.
25– 34% with 10 year survival. Less infiltrative and complete surgical excision
possible.
III. Ependymoma :-
Arise from spinal cord especially from lumbo-sacral region in adults and
from ventricles especially fourthventricle in children.
Histologically myxopapillary that is, papillary arrangement of cells and mucin
production. Usually relatively demarcated from adjucent neural tissue.
Metastasis through CSF occurs.
Gross total excision provides 5 year disease free survival in 80% cases.
IV. Germinoma :-
A variety of germ cell tumor arising in midline structures.Common site
within or adjacent to 3rd ventricle. Due to their location causes features of
hypothalamic dysfunction like diabetes incipedus, visual field defects,
disturbances of memory and hydrocephalus.
Radiosensitive and chemosensitive. 5 year survival in 80% patients.
V. Medulloblastoma :-
Arise from neural precurssor cells. The most frequent malignancy of
children. Rapidly growing tumours affecting vermis of the cerebellum and giving
rise to wide spread metastasis.
VI. Meningioma :-
Arise from arachnoid cells particularly seen in sites having arachnoid
granulations. Those are usually benign and attached to dura. More common in
women. Invades skull rarely invades brain.
Common sites are along sagital sinus, c-p angle and along the dorsum of spinal
cord.
Treatment : Surgical resection and post – operartive radiation.
VII. Schwannoma :-
Arise from Schwann cells of nerve roots. Commonly from 8th cranial nerve and
less commonly 5th cranial nerve is affected. It can arise from any cranial nerve
except optic and olfactory (myelinated by oligodendroglia). Neurofibromatosis
type – II predisposes to vestibular schwannoma. Neurofibromatosis type – I
predisposes to schwannoma of spinal nerve roots.
Clinical features are progressive unilateral hearing loss, tinitis, vertigo.
Treatment : Surgical excision.
VIII. Craniopharyngioma :-
Arise from remnants of the pituitary stalk called Rathke’s pouch
(mesodermal structures from which anterior pituitary gland is derived). Cystic
supracellar tumour and in adults usually calcified.
Clinical features are growth failure in children, endocrinal disturbances due to
pressure on hypothalamus like diabetes incipedus, somnolence, obesity,
hyperphagia and visual loss.
METASTATIC TUMORS OF BRAIN :-
Common route is through haematogenous.Primary site is lung in most of
the cases. Usually from carcinoma breast metastasis occurs to cerebellum and
posterior pituitary gland. Others are GIT malignancies, melanoma, thyroid
cancer, Hodgkin’s lymphoma. In brain the usual site of metastasis is the grey
matter – white matter junction and border zone between middle cerebral and
posterior cerebral artery distribution. Usually incurable. Palliative therapy
and radiotherapy are the treatment of choice.
INVESTIGATIONS :-
In primary brain tumour no increase in ESR and tumor specific antigen.
In metastatic tumours associated with systemic signs of malignancy.
Lumbar puncture – Should not be performed in patients with mass lesion it may
precipitatebrain herniation.
CSF : increase opening pressure, elevated protein level, mild lymphocytic
pleocytosis and rarely contains malignant cells.
EEG : to distinguish epileptic seizures produced by focal lesions and idiopathic
epilepsy.
CT Scan, MRI, PET, SPECT |
