PATHOLOGY
OF C.N.S
Central
nervous system is
Composed
mainly of brain and spinal cord
The
skull and vertebrae form a rigid compartment protecting the delicate CNS
This
Rigidity has serious disadvantages
When
there is an expanding lesion
Pressure
mounts inside the cranium
With
compression of the normal brain tissue
Meninges
and CSF
The
CSF circulates freely in the subarachnoid space over the whole CNS
The
ventricular system acts as a protective water bath
Dxs
at this site e.g. infections, are usually widespread over brain & cord
Impediment
to CSF flow causes hydrocephalos
Meninges
& CSF cont
Extradural
lesions tend to be localised bc they have to strip the dura from bone
Subdural
lesions remain local but can spread more widely bc arachnoid & dura are
loosely attached
Arachnoid
is a delicate membrane which sends trabeculae across the subarachnoid space
which contains CSF & blood vessels
Dxs
in the subarachnoid space are prevented from penetrating the brain by the Pia
matter
Parietal
surfaces of cerebrum covered by meninges
Base
of the brain
Sulci
and gyri
Base
of the brain
Cerebellum
& brain stem
CNS
CELLS
NEURONS:
aggregates - nuclei, ganglia or elongated columns or layers – intermediolateral
gray column or cerebral cortex
GLIA:
Macroglia – astrocytes, oligodendrocytes, ependyma or microglia – fixed
macrophage system
PATHOLOGY
OF THE C N S
Increased
intracranial tension/herniations
*definition: CSF pressure
above 200mm of water (15mmHg) with the patient in lateral decubitus position
*causes: The causes include increased CSF
production,decreased csf drainage, haemorrhage, tumours, cerebral oedema,
cerebral abscess
*clinical
features: Head
ache that is worse in the mornings, mental slowness, confusion, papillaedema,
focal seisures from causative lesion.
*morphology: Flattening of
the gyri and obliteration of the sulci, herniations such as tentorial,
subfalcine uncinate, tonsilar. Duret haemorrhages.
CEREBRAL
OEDEMA
Vasogenic
oedema: Is
the accumulation of oedema fluid in the interstitial space and this is the most
common type of cerebral oedema. It is due to capillary damage or formation of
new capillaries; eg, around tumours, abscesses infarcts, etc
Cytotoxic
oedema: Is
the accumulation of excess intracellular water. It predominantly affects gray
matter and occurs usually due to processes such as ischaemia and water
intoxication.
Interstitial
oedema: This
is seen in non-commumunicating hydrocephalus. The fluid accumulates around the
cerebral ventricles by crossing the ependymal lining
HYDROCEPHALUS
Most cases are due to blockage to csf flow along its pathway
Most cases are due to blockage to csf flow along its pathway
A-COMMUNICATING
*CSF
overproduction as in choroid plexus papilloma
*Deficient
reabsorption as in meningitis, sinus thrombosis, subarachnoid haemorrhage
B-NON-COMMUNICATING
Congenital
malformations such as stenosis of the aquiduct of sylvius, forking of the
aquiduct, gliosis of aquiduct, Dandy-Walker malform., Anold-Chiari malform.,
etc.
Neoplasms
Ependymoma of IV ventricle
Choroid plexus papilloma
Medulloblastoma, Cyst of IV ventricle
Inflammation.
Meningitis, cerebella abscess, CMV
Haemorrhage
such intraventricular, epi and subdural and intraparenchymal.
Hydrocephalus
ex-vacuo
INFLAMMATIONS OF THE CNS
MENINGITIS
Defn.
This is an inflammatory process of the CNS coverings due to infectious
or Chemical agents or cancer deposits
( carcinomatous meningitis)
Types:
Infection, Chemical and carcinomatous
Infections:
BACTERIAL
VIRAL
FUNGAL
Routes
of infection of the CNS:
Blood stream
Direct implantation
(sharp object or skull # )
Local extension (ENT,
Ophthal, Dental, etc)
Peripheral nervous
system (Rabies, polio, etc)
Bacterial
infections
ORGANISM PEAK AGE INCIDENCE GRAM STAIN
Escherichia coli/grp B strept Neonates Gram negative rods
Hemophilus influenzae Infants and Children Gram negative coccobacilli
Now
strept pneumon b/c of immunisation
Neisseria meningitidis Adolescents and Young adults Gram negative diplococci
Streptococcus pneumoniae Older adults or Children Gram positive cocci in chains
Acute
pyogenic meningitis
Causative
agents:
E
Coli, H Influenza, Neisseria meningitidis, pneumococcus
Neisseria
meningitidis is the cause of epidermic meningitis among adults and adolescents.
Epidemic
meningitis (CSM)
-It occurs in
five-yearly epidermics with peaks of severity every 15-20 years.
-Severity
of the epidermics decreases south-wards towards the costal regions of Nnigeria
-the
pattern of disease is influenced by successful immunisation of the population
and the use of antibiotics
-it
is transmitted by droplet infection
-the
infective organism has been predominantly type A until recently when types B
and C were recognised. These types respond less well to sulphonamides
-the
organism most frequently inhabits the nasopharinx and gets to the CNS via blood
-clinical
aspects include positive Kernig’s and Brudzinki’s signs, fever, features of
toxicity, peticheal haemorhhages in the skin, etc.
-shock
may occur secondary to adrenal haemorrhage (Waterhouse-Fredrickson syndrome)
Pyogenic
menin.
-DIC
can occur
-arthritis
and vasculitis secondary to immune complex deposition may also occur
-hypocomplementaemia
(C3 particularly) is often classic
-diagnosis:
csf is hasy or purulent & is under high pressure with white cell count of
900,000/mm3 and sugar content is usually low, protein content is
usually high
-smear
will show intracellular lanceolate diplococci.
-gross
morphology; purulent exudate over the vertex; microscopically, pmn & pus
cells in leptomeninges with venulitis, leptomeningeal thickening.
-Complications—
cerebral abscess, adhesive arachnoiditis, hydrocephalus, cranial nerve palsies
(especially in Tb meningitis), mental deficiency especially in
meningoencephalitis
Acute
lymphocytic meningitis (ALM)
-this is a viral
meningitis presenting clinically as acute pyogenic meningitis
-csf
findings are different from those of csm; lymphocytosis rather than pmn, csf
sugar is normal with moderate protein elevation.
-it
is self limiting
-Organisms
involved include ECHO viruses, Coxsackie, EBV and HSV
Chronic
meningitis (Tbc & Syphilis)
The
archi-type is Tbc meningitis and is usually 20 to a 10
elsewhere
Other
causes of chronic meningitis include cryptococcus neoformans,, brucella and
treponoma pallidum
Grossly,
there is gelatinous or fibrinous exudate at the base (basal meningitis), other
cause of basal meningitis is H influenza meningitis
Focal
granularities may be present
Tuberculoma(s)
may develop in the parenchyma
Microscopy;
lymphocytes, plasma cells, Macrophages, granulomata, obliterative arteritis
(end arteritis obliterans)
Csf
shows pleocytosis (1000 cells/mm3), normal is 100 cells/mm3 very
high protein content and mildly low sugar
Cryptococcal
meningitis gives a slimy exudate (microscopically as soap bubbles)
Clinically;
malaise, Hd ache, mental confusion, vomiting
Neurosyphilis
Is
the tertiary stage of syphilis and occurs in about 20% of untreated pts
Occurs
in the form of meningovascular neurosyp, paretic neurosyp and tabes dorsalis
Meningovascular
neurosyp usually
involves the base of the brain and variably convexities and cord meninges
There
may be associated endarteritis (Heuner arteritis)
Cerebral
gummas may occur (plasma cell-rich mass lesions) and neuronal loss
Paretic
type occurs
due to cerebral invasion by T Pallidum terminating into sever dementia (general
paresis of the insane)
Tabes
dorsalis is
the result of damage by spirochetes to the sensory nerves leading to locomotor
ataxia and Charcot pains (loss of pain sensation to skin and and joint damage
There
is loss of axons and myelin with pallor and atrophy in dorsal columns of cord.
Organism are not usually demonstrable in the cord lesions
Pts
with HIV infection are at a higher risk of neurosyphilis
Patients
with nurosyphilis may come with incomplete or mixed pictures of the three types
Encephalitis:
This simply means inflammation of the brain
This simply means inflammation of the brain
Is
divided into:
Bacterial; Mainly Tb. &
syphilis (in the form of neurosyphilis), brain
abscess.
Viral; Rabies, CMV, HIV,
Polio, Herpes simplex,
Arboviruses (EEE,WEE,
Venezuela, etc)
Brain
abscess: This can be due to direct implantation, haematogenous (sepsis, SBE,
cyanotic heart disease) or local extension. Complications include herniation,
ventriculitis, sinus thrombosis, meningitis, etc.
Slow
viral diseases of the CNS:
The agents that cause these diseases have a long latent period, the disease evolves very slowly and does not clinically resemble acute viral Dx.
The agents that cause these diseases have a long latent period, the disease evolves very slowly and does not clinically resemble acute viral Dx.
Divided
into: a)
those with known viral cause (SSPE, PML, PRP
= progressive rubella panancephalopathy)
b) those with no well xrised cause (unconventional agent= spongoform) such
as Kuru dx and Creutzfeldt-Jacob dx
(also called Prion Protein-PrP diseases). This agent is now known to be both
transmissible and infectious
SSPE: -Is
caused by measles virus
-also called Dawson’s encephalitis
-always preceded by attacks of
measles in distant past or immunisation.
Morphology; -perivascular lymphocytic
infiltrates & plasma cells
-neuroglial and neuronal
loss
-dense gliosis
-inclusion bodies in
oligodendroglia are usually present.
Slow virus
infection cont.
PML
(progressive
multi-focal leukoencephalopathy)
Viral infection
of oligodendroglia and their destruction
It causes demyelination
as its principal effect
It occurs in
association with advanced haematological malignancies and immunodeficiency
states
It is caused by JC
virus and SV40
Morphology:
Sunken areas in white matter
Microscopy:
Demyelination
Inclusion bodies
in oligodendroglia
Xtic giant
astrocytes
Strikingly little
inflammatory reaction
There is sparing
of the gray matter
TUMOURS
OF THE C N S
Divided into primary and secondary
Divided into primary and secondary
CLASSIFICATION
(Modified WHO)
•
Tumours
of neuroglia:
a) Astrocytes -astrocytoma: anaplastic
GBM
pilocytic
b) Oligodendrocytes -Oligodendroglioma
c) Ependyma and its homologues ependymoma myxopap & sub.
choroid
plexus papilloma
•
Tumours
of neurones Neuroblastoma
Ganglioneuroblastoma
Ganglioneuroma
CNS
tumour classification cont.
3
Tumours of neurones and neuroglia -Ganglioglioma
4
Tumours of primitive undifferentiated cells - -Medulloblastoma
5
Tumours of pineal cells -Pinioloma
& pineocytoa
6
Tumours of meninges -Meningioma,
meningeal haemangioma
7
Tumours of nerve sheath cells -Schwannoma
& neurofibroma
8
Lymphoma -primary and secondary
9
Malformative tumors -Craniopharyngioma, epidermoid cyst, colloid cyst
10
Metastatic tumours.
Four
major classes of brain tumours
Gliomas
Neural
tumours (Gangliocytomas, gangliogliomas)
Poorly
differentiated neoplasms
meningiomas
Properties
of C N S tumours
A)
Biological properties: Biologic malignancy/histologic malignancy
A benign tumour at strategic location
may prevent surgical removal and this is what is meant by biologic malignancy
eg. Ependymoma of the floor of the IV ventricle or a meningioma around the
carotid artery.
A malignant tumour shows infiltrative
margins hence complete removal without extensive removal of brain tissue is
rarely possible.
Some tumours show intraneural seeding
via the CSF such as medulloblastoma and some astrocytomas leading to
carcinomatous meningitis.
. B) Clinical effects: Local; depends on site and size.
General;
insiduous frontal lobe tumour may grow large
before coming to clinical attention
. C) Incidence and distribution:
-CNS tumours are one of the
commonest tumours in infants and children.
-CNS tumours are unusual above
the age of 70 years
-Some of them have
predisposition to some sites such medulloblastoma which is -usually confined to cerebellum and pilocytic
astrocyto. to hypothal. and cerebel.
-70% are infratentorial in
children; reverse is the case with adults
-age specificity;
medulloblastoma is seen in the 1st
2 decades of life.
NEUROGLIAL
TUMOURS
Astrocytoma
and GBM.
-they
form 80% of adult primary brain tumours
-three
grades of increasing anaplasia -asrocytoma;
fibrillary, protoplasmic
& gemistiocytic
-anaplastic
-Glioblastoma
multiforme
-they
tend to be more anaplastic with time
-misleading
diagnosis can arise from small biopsies of anaplastic tumours
-they
are poorly defined
-they
can be solid, soft, gelatinous or firm depending on fibrillary content
-xtic
fibrillary background of astrocytic processes of varying density and calibre.
Astrocytomas
cont.
-GBM almost never arise from the
cerebellum
-anaplastic
variants have in addition hypercellularity, pleomorphism, nuclear
hyperchromasia and irregularity.
-GBM
has a variegated appearance, necrosis, cyst & endothelial cell prolif. are
common
-microscopically shows necrosis and
pseudopallisading in addition to other features of anaplasia.
-bizarre giant cells may be
present
-prognosis is very poor.
- GLIOMATOSIS CEREBRI – infil of brain by
neoplastic astrocytes
Pilocytic
astrocytoma:
-almost
invariably benign
-occurs
typically in children and young adults
-usually
located in the cerebellum
-is
composed of hypercelluar bipolar cells with long hair-like processes
-Rosenthal
fibres and microcysts are present
CNS
tumours cont.
Oligodendroglioma:
-forms
about 5% of gliomas
-mostly
cerebellar in location
-most
common in middle life
-circumscribed
gelatinous gray masses often with cysts, calcification, etc.
-microscopically
sheets of regular cells with spherical nuclei surrounded by cytoplasmic halo
-xtic
fried egg appearance
-calcification
is present in 90% of cases.
-etc
Meningioma
Predominantly
benign tumours of adults
Arise
from meningothelial cells
Usually
attached to the dura matter
May
be found along any of the external surfaces of the brain
Usually
round to oval well defined encapsulated masses with compressive effects on the
underlying brain
Variant
called meningioma en plaque has a flat growth patter
Has
up to four grades (I-IV) with varying degrees of risk of recurrence
Varying
histological pattern with no prog. Significance; fibroblastic, syncytial,
transitional, etc.
Psammoma
bodies are common in a variant called psammomatous meningioma
Atypical
(WHO II/IV) also called aggressive and
Anaplastic (malignant) meningiomas have varying grades of histology that change
with degree of aggression.
Medulloblastoma
This
tumour occurs predominantly in children and exclusively in the cerebellum
One
of the small blue cell tumours of childhood
The
tumour is largely undifferentiated
Morphologically
located mainly in the midline of the cerebellum
Rapid
growth may lead to hydrocephalus
Often
well circumscribed, gray and friable
Microscopically
shows extreme cellularity with sheets of anaplastic cells with scanty cytoplasm
Mitoses
are abundant
Direct
dissemination through CSF (‘drop metastasis’) occurs
The
tumour is highly malignant and prognosis is dismal
It
is highly radiosensitive
Primary
CNS lymphoma (PCNSL)
Accounts
for 2% of extranodal lymphomas and 1% of intracranial tumours
Commonest
intracranial neoplasm in the immunosuppressed
Often
multiple sites in the brain at presentation
Extracranial
involvement is a rare and late complication
Majority
are of B-cell origin
Relatively
aggressive disease with poor response to chemo.
Morphologically,
the lesions are often multiple and involve deep gray matter and white matter
Nearly
always high grade and cells accumulate around blood vessels giving typical hooping
which is xtic of PCNSL
CNS
MALFORMATIONS AND DEVELOPMENTAL DISEASE
Aetiology
and pathogenesis, not clear however genetic and environmental factors clearly
play significant role.
NEURAL
TUBE DEFECTS
Failure
of a portion of neural tube to close may lead to several malformations
involving combination of neural tissue, meninges or overlying bone or soft
tissues.
ANENCEPHALY
Is a
malformation of the anterior end of the neural tube with absence of brain and
calvarium
It
occurs in 1 to 5 per 1000 live births forebrain devt. Is disrupted and what
remains is only area cerebrovasculosa
ENCEPHALOCELE
Is a
diverticulum of malformed CNS tissue extending through a cranial defect
Is
mostly occipital in location
SPINAL
DYSRAPHISM OR BIFIDA.
From asymptomatic bony defect to severe malformation with flattened and
disorganised segment of spinal cord associated with outpouching of meningeal covering
MENIGOCELE/MENINGOMYELOCELE- Meningeal/neural tissue extrusion
Miningomyelocoele
FOREBRAIN
ABNORMALITIES
Polymicrogyria
Is
characterised by loss of neural external contour of the cerebral convolusions
The
gyri appear small, numerous and poorly formed
Meganencephaly/microencephaly.
These refer to the abnormality in volume of the brain. Alcoholism (fetal
alcohol syndrome), genetic defects and HIV infection acquired in utero may lead
to micoencephaly.
Agenesis
of corpus callosum
Relatively
common malformation is the absence of the white matter bundles that carry
cortical projections btw the two cerebral hemispheres
POSTERIOR
FOSSA ABNORMALITIES
Anold-Chiari
malformation consist of small posterior fossa, a misshapen midline cerebellum
with downward extension of the vermis through foramen magnum with consequent
hydrocephalus, etc.
Dandy-Walker
malformation is characterised by an enlarged posterior fossa. The cerebellar
vermis is either absent or rudimentary. A midline cyst may replace it.
SYRINGOMYELIA
AND HYROMYELIA.
Hydromyelia.
Characterised by discontinuous multisegmental or confluent expansion of the
central canal of the spinal cord
Syringomyelia.
Fluid-filled cleft-like cavity in the inner portion of the cord
Flattened
cerebellum, elongation of brain stem, herniation into a conical shaped foramen
magnum
Hypertensive
vascular diseases of the CNS
Binswanger’s
dx; also called multi-infarct dementia (mainly involving white matter),
characterised by dementia, gait abnormalities, and pseudobulba signs. It is
usually due to cerebral athreosclerosis, vessel thrombosis or embolism, or
cerebral arteriolar sclerosis from HPTN
Lacunae/lacunar
infarcts; single or multiple small infarcts due to cerebral arteriolar
sclerosis in HPTN leading to development of small cavities or lakes (etat
lacunaire). Most commonly seen in basal ganglia and hemispheric white matter
Hypertensive
encephalopathy- Is due to failure of autoregulation of blood flow with break
down of BBB. Is Xrised by head ache, drowsiness, vomiting, convulsions, stupor,
coma. Pathologically, there is cerebral oedema, peticheal haemorhages, fibrinoid
necrosis of arterioles. These changes are also seen in eclampsia, hypertension
of acute nephritis, and malignant hypertension.
Primary
demyelinating diseases of the CNS
These
are acquired conditions characterised by preferential damage to myelin with
relative preservation of axons. These include:
Multiple
sclerosis
Acute
disseminated encephalomyelitis (measles, chickenpox, rubella, etc)
Central
pontine myelinosis (demyelination
in the basis pontis and is associated with many factors such as alcolism, rapid
correction of hyponatraemia, etc)
Leukodystrophies
.represent
a group of dxs in which there is an intrinsic defect that interferes with
generation and/or maintenance of myelin
Multiple
sclerosis
Is
the commonest demyelinating dx of the CNS
Is
commoner in temperate climates and people of European extraction
It
affects young adults (peak btw 18-40 years)
Prevalence
is approximately 1 per 1000 persons in the US and Europe
Xrised
by waxing and waning neurological abnormalities involving different regions of
the CNS over a number of years
Aetiology:
it is an autoimmune disorder characterised by destruction of myelin through
highly sensitized T-cells. The lesion contains CD-4 and CD-8 lymphocytes as
well as macrophages and are reactive to MBP
Current
evidence suggests that infections and hereditary factors contribute to the
autoimmunity of the dx.
Morphology
of multiple sclerosis
The external
appearance of the brain and spinal cord is usually normal.
Cut
sections are xrised by plaques (areas of demyelination)
The
plaques may appear anywhere in the brain and this may explain the wide variety
of the clinical features.
Common
sites include periventricular white matter, the optic nerves and spinal cord.
The
plaques are well demarcated with acute lesions appearing slightly pink and soft
while older lesions tend to be firm and pearly gray to pink
Microscopically
the lesions are xrised by demyelination initially as perivenous distribution
accompanied by variable perivascular lymphocytic inflammatory infiltrate.
Evidence
of myelin breakdown is present in active lesions manifested by lipid laden
macrophages
The
peripheral nervous system is spared.
Clinical
features of MS
Onset
may be acute or insiduous
The
clinical manifestations are protean
Common
manifestations include visual disturbances (blurred vision, diplopia,
scotomata), paraesthesias, spasticity of one or more extrimities, speech
disturbances and gait abnormalities.
Various
emotional disturbances may be seen but intelectual function is typically
preserved.
The course
of MS is unpredictable with some pts dying within weeks to months of onset
and others experiencing a normal life span.
However
in most cases the dx is xrised by multiple exacerbations and remissions
with cumulative neurological deficits developing over the course of years.
DEGENARATIVE
DISEASES
These
are diseases of gray matter principally characterised by progressive loss of
neurons with associated secondary changes in white matter tracts
The pattern
of neuronal loss is selective with some areas affected more than others and in
fact some remain unaffected
The
diseases arise without any clear inciting event in pts without previous
neurologic deficits
The
diseases are selective in areas of affectation, eg; some are cortical
while others may simply be subcortical
They
also have many shared features
A
common theme among them is the development of protein aggregates that are resistant
to normal cellular degredation systems
Some
examples of these diseases include:
1 Alzheimer disease (cortical)
2 Pakinsonism/Pakinson disease (Basal ganglia
& Brain stem)
3 Huntington disease (Basal ganglia &
Brain stem), etc.
ALZHEIMER
DISEASE
Is
the most common cause of dementia in the elderly
Is
a degenerative disaese of the CNS
Most
cases occur after the age of 50 years with increasing incidence as age advances
Most
cases are sporadic but about 10% have family history of dementia
Clinical
features include progressive impairment of memory and other cognitive functions
independent of the state of attention, and death is usually as a result of
bronchopneumonia or other infections
The
so-called "early onset" cases of AD in persons in their 30's, 40's,
and 50's may have a genetic basis. Less than 1% of early onset AD cases are
linked to a genetic defect on chromosome 21 (which may explain the appearance
of Alzheimer's disease in persons with Down syndrome surviving to middle age)
which affects amyloid precursor protein, resulting in fibrillar aggregates of
beta-amyloid that is toxic to neurons. About half of early onset AD cases are
linked to mutations in the presenilin 1 gene on chromosome 14. A presenilin 2
gene has been discovered on chromosome 1, but this defect accounts for less
than 1% of cases.
Alz
cont….
The
more typical "late onset" cases of AD occurring after age 60 may have
underlying genetic defects. A genetic locus on chromosome 19 encodes for a
cholesterol transporter called apolipoprotein E (apoE). The E4 variant of apoE,
which increases deposition of fibrillar beta-amyloid, can be found in 40% of AD
cases. A genetic locus on chromosome 12 that encodes for alpha-2-macroglobulin
may be found in 30% of AD cases.
Alz
cont…
The
definitive diagnosis is made pathologically by examination of the brain at
autopsy. Grossly, there is cerebral atrophy, mainly in frontal, temporal, and
parietal regions. As a consequence, there is ex vacuo ventricular dilation.
Microscopically,
there are neurofibriallary tangles, neuritic plaques, amyloid (congophilic)
angiopathy, hirano bodies and granulovacuolar degeneration
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July 11, 2015
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