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Category Archives: Brain
Alzheimer’s Disease Pathology
Alzheimer’s Disease Pathology
Alzheimer’s disease gross and light microscopic features
Gross – variable degree of cortical atrophy with widening of the cerebral sulci that is msot pronoucned in the frontal, temporal, and parietal lobes
- with significant atrophy, there is compensatory ventricular enlargement secondary to loss of parenchyma
LM – neurofibrillary tangles, senile (neuritic) plaques, amyloid angiopathy
- neurofibrillary tangles: bundles of filaments in the cytoplasm fo the neurons that displace or encircle the nucleus
- often have an elongated “flame” shape
- in some cells, the basket weave of fibers around the nucleus takes on a rounded contour (globose tangles)
- visible as basophilic fibrillary structures with H&E staining but dramatically demonstrated by silver (Bielschowsky) staining
- commonly found in cortical neurons, especially in the entorhinal cortex, as well as in otehr sites such as pyramidal cells of the hippocampus, the amygdala, the basal forebrain, and the raphe nuclei
- tangles insoluble and apparently difficutl to proteolyzxe in vivo, thus remaining visible in tissue sections as “ghost” or “tombstone” tangles long after the death of the parent neuron
- stain with tau, ubiquitin, amyloid b-peptide (Ab)
- neuritic plaques: focal, spherical collections of dilated, tortuous, silver-staining neuritic processes (dystrophic neurites) surrounding a central amyloid core, often surrounded by clear halo
- range in size from 20-200 mm in diameter
- microglial cells and reactive astrocytes present at their periphery
- found in hippocampus and amygdala as well as in neocortex
- usually relative sparing of primary motor and sensory cortices (this also applies for neurofibrillary tangles)
- amyloid core can be stained by Congo red and Bielschowsky silver methods
- amyloid core contains several abnormal proteins, stains with Ab
- Ab immunostaining demonstrates existence, in some patients fo amyloid peptide deposits of lesions lacking the surrounding neuritic reaction
- these lesions called diffuse plaques, found in superficial portison fo cerebral cortex as well as in basal ganglia and cerebellear cortex
- commonly when diffuse plaques found in cerebral cortex, they appear to be centered on small vessels or on clusters of neurons
- diffuse plaques may represent early stage of neuritic plaque development
- amyloid angiopathy almost always present
- vascular amyloid derived from same precursor as amyloid cores of plaques (APP)
- granulovacuolar degeneration: formation of small (5 mm) clear intraneuronal cytoplasmic vacuoles, each of which contains an argyrophilic granule
- found in great abundance in hippocampus and olfactory bulb in Alzheimer’s
- Hirano bodies: elongated glassy eosinophilic bodies consisting of paracrystalline arrays of beaded filaments, with actin as major component
- found most commonly along hippocampal pyramidal cells
Alzheimer’s disease clinical features
initially – forgetfulness and other memory disturbances
- insidious impairment of higher intellectual function
- alterations in mood and behaviour
with progression – language deficits (aphasia)
- disorientation
- loss of mathematical skills
- loss of learned motor skills
final stages – incontinence
- muteness
- inability to walk
common terminal event – pneumonia
Alzheimer’s disease pathogenesis
- see above
Alzheimer’s disease gross features of the brain
- cortical atrophy
- widening of cerebral sulci (most severe in frontal, temporal, parietal lobes)
- ventricular enlargement
Alzheimer’s disease microscopic features of the brain
- neurofibrillary tangles
- senile (neuritic) plaques
- amyloid angiopathy
- diffuse plaques
- granulovacuolar degeneration
- Hirano bodies
Diagnostic criteria
- neurofibrillary tangles, senile (neuritic) plaques, amyloid angiopathy can all be seen to a lesser extent in brains fo elderly nondemented individuals
- diagnosis of Alzheimer disease based on a combination of clinical and pathologic features
- several different methods proposed, which include evaluation of different regions of the brain and various methods for estimating the frequency of plaques and tangles
References:
1. Robbins & Cotran Pathologic Basis of Disease, 8th edition. Vinay Kumar, MBBS, MD, FRCPath; Abul K. Abbas, MBBS; Nelson Fausto, MD; Jon Aster, MD. Saunders. Published June 2009.
2. Sternberg’s Diagnostic Surgical Pathology, 5th edition. Darryl Carter, Joel K. Greenson, Victor E. Reuter , Mark H. Stoler. Lippincott Williams & Wilkins. Published Aug 26 2009.
Parkinson’s disease
Parkinson’s disease
- degeneration of dopaminergic neurons in substantia nigra
Gross appearance:
- loss of pigmentation in substancia nigra and locus ceruleus
Microscopy
- loss of cholinergic neurons
- astrocytic gliosis
- accumulation of neuromelanin in macrophages
- Lewy body inclusions → dense core surrounded by a clear halo→ IHC: α-synuclein and Ub positive
- substancia nigra, locus ceruleus, nucleus of Meynert
Posted in Brain
Tagged dopaminergic neurons, Lewy body inclusions, locus ceruleus, loss of cholinergic neurons, nucleus of Meynert, Parkinson's, Parkinson's disease, substancia nigra, substantia nigra
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Alzheimer’s Disease
Alzheimer’s Disease
Clinical
- late-onset sporadic, familial (early, late),
- familial Alzheimer’s disease is associated with trisomy 21 (extra copy of APP results in ↑ amyloid β peptide
Pathology
Gross
- cortical atrophy in cortical, parietal, and temporal lobes
- ventricles enlargement
Microscopy
1. Neurofibrillary Tangles:
- aggregates of microfilaments in the cytoplasm of neurons, displace nucleus → flame shape
- hyperphosphorylated “paired helical filaments” such as tau, MAP, Ub, amyloid β peptide
→ frequently ubiquitinated
- found in pyramidal cells, often flame-shaped, globular filamentous shape
- hippocampus, amygdala
2. Senile plaques:
-structure = clear halo and dystrophic neurites and central amyloid core (amyloid β peptide)
- diffuse plaques smaller dense amyoid cores only
- hippocampus, amygdala
3. Amyloid angiopathy
4. Granulovacuolar degeneration
- cytoplasmic granules in pyramidal neurons (hippocampus)
5. Hirano bodies
- glassy, eosinophilic body in pyramidal neurons (hippocampus)
Culprits
1. amyloid β peptide is a secretase product of amyloid precursor protein
2.presenilins 1 and 2 on chromosomes 14 and 1 lead to increased amyloid β peptide and early onset familial Alzheimer disease
3. Apolipoprotein E on chromosome 19 → mechanism unclear
Posted in Brain
Tagged Alzheimer's Disease, Alzheimers, amyloid, Amyloid angiopathy, amyloid peptide, amyloid precursor protein, amyloid β, amyloid β peptide, Apolipoprotein E, familial Alzheimer's disease, Granulovacuolar degeneration, Hirano bodies, Neurofibrillary Tangles, Senile plaques, Sporadic Alzheimer's Disease, Trisomy 21
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Creutzfeld-Jakob Disease
Creutzfeld-Jakob Disease
Causes of Creutzfeld-Jakob disease
• Due to abnormal folding of prion protein (PrP) from α-helix to β-pleated sheet
• May be genetic or acquired
• Accumulation of abnormally folded prion protein in neural tissues causes cytoplasmic vacuoles and eventual neuronal death although mechanism is still unknown
Creutzfeld-Jakob disease clinical manifestations
• Initial subtle changes in memory and behavior followed by rapidly progressive dementia
• Startle myoclonus (involuntary jerking muscle contractions on sudden stimulation)
• Cerebellar dysfunction, manifesting as ataxia
• Peak incidence in seventh decade (familial CJD: Valine at codon 129 with D178N mutation of PRNP gene)
• vCJD occurs in young adults with behavioural symptoms featured more prominently and a slower progression to dementia
Creutzfeld-Jakob disease gross and microscopic findings
• Disease is so rapid, there is little atrophy of the brain
• Spongiform transformation of cerebral cortex and deep gray matter structures (caudate, putamen)
• A multifocal process that results in uneven formation of small, apparently empty microscopic vacuoles of varying size in neuropil and perikaryon of neurons
• Advanced cases demonstrate neuronal loss, gliosis, and expansion of vacuolated areas into cyst-like spaces (“status spongiosus”)
• No inflammatory infiltrate is present
Alzheimer’s
Alzheimer’s disease
Alzheimer’s Clinical Features
• Forgetfulness and other memory disturbances
• Language deficits
• Loss of mathematical skills
• Loss of motor skills
• Personality changes
Alzheimer’s Pathogenesis
• Aβ is thought to be the critical molecule in the pathogenesis of Alzheimer’s dementia
• Aβ is a peptide that aggregates readily, forms β-pleated sheets, elicits a response from astrocytes and microglia and is neurotoxic
• Aβ is generated from amyloid precursor protein (APP), a protein of uncertain function that is expressed on the cell surface
• Cleavage of APP by β-secretase and γ-secretase, generating Aβ (thought to occur physiologically in order for cell signalling and transcriptional regulation)
• Mutations in PS1 and PS2 (genes that encode for portions of the γ-secretase enzyme) also lead to accumulation of Aβ, and are responsible for forms of familial Alzheimer dementia
Alzheimer’s Brain Features
• Cortical atrophy
• Sulcal widening (pronounced in frontal, temporal and parietal lobes)
• Compensatory ventricular enlargement (hydrocephalus ex vacuo)
Alzheimer’s Histology
• Neuritic plaques
• Neurofibrillary tangles
• Cerebral amyloid angiopathy
• Granulovacuolar degeneration
• Hirano bodies
Meningioma
Meningioma
Gross features
• Rounded mass, well-defined dural base, may extend into overlying bone (en plaque variant may extend sheet-like along dural surface)
• Surface of mass is encapsulated with fine, fibrous tissue; may have bosselated or polypoid appearance
• Tumour may be firm, fibrous and finely gritty or may be extremely calcified; does not contain necrosis or hemorrhage
Histologic subtypes
• Syncytial
• Transitional
• Fibroblastic
• Microcystic
• Papillary
• Psammomatous
• Rhabdoid
• Secretory
• En plaque variant
• Atypical
• Anaplastic (malignant)
Features suggesting aggressive meningioma behaviour
• High mitotic index (>4 mitoses per 10 HPF: atypical; >20 mitoses per 10 HPF: anaplastic)
• Increased cellularity
• Small cells with high N:C ratio, prominent nucleoli
• Patternless growth
• Necrosis
• Clear cell/chordoid morphology (Grade II/IV)
• Papillary/Rhabdoid morphology (Grade III/IV)
Meningioma immunohistochemistry and differential diagnosis
• EMA (positive in meningiomas)
• Cytokeratin (positive in secretory meningiomas)
• CEA (positive in secretory meningiomas)
Posted in Brain
Tagged Aggressive meningioma, Meningioma, Meningioma diagnosis, Meningioma differential diagnosis, Meningioma immunohistochemistry
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Neurofibromatosis
Neurofibromatosis
Associated genetic changes
1. Neurofibromatosis type 1: autosomal dominant genetic disease involving mutation of NF1 gene, encoding neurofibromin, a tumour suppressor involved in signal transduction
2. Neurofibromatosis type 2: autosomal dominant genetic disease involving mutation of NF2 gene, encoding merlin, a tumour suppressor, with similarities to cytoskeletal proteins. It is thought to mediate contact inhibition and proliferation of Schwann cells.
Essential diagnostic lesions
1. Neurofibromatosis type 1
1. Neurofibromas (plexiform, solitary)
2. Lisch nodules of the iris
3. Café-au-lait spots
2. Neurofibromatosis type 2
1. Bilateral acoustic schwannomas
2. Multiple meningiomas
3. Gliomas (typically ependymomas of the spinal cord)
4. Schwannomatosis
5. Meningioangiomatosis
6. Glial hamartia
Associated malignancies
1. MPNST
2. Rhabdomyosarcoma
3. Wilm’s tumor
4. CML
5. Meningiomas
6. Optic nerve gliomas/JPA
7. Pheochromocytomas
Plexiform neurofibroma
1. Diffuse involvement of subcutaneous tissue containing numerous, tortuous, thickened nerves
2. Proliferation of all elements of peripheral nerve (neurites, Schwann cells, and fibroblasts)
3. Dispersed in loose, disordered, myxoid stroma (shredded-carrot appearance)
Posted in Brain
Tagged , Cafe-au-lait spots, Lisch nodules, Merlin, Neurofibromas, Neurofibromatosis, Neurofibromatosis type 1, Neurofibromatosis type 2, Neurofibromin, Plexiform Neurofibroma
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Parkinson’s disease Parkinson’s disease
Parkinson’s disease
Parkinson’s disease pathogenesis
1. Degeneration of dopaminergic neurons of substantia nigra projecting to striatum (causes loss of striatal dopaminergic content)
Gross morphology of the Parkinson’s disease brain
1. Pallor of substantia nigra and locus ceruleus
Mutation responsible for the hereditary form of Parkinson’s disease
1. Mutations in alpha-synuclein (autosomal dominant form)
2. Mutations in parkin (juvenile autosomal recessive form)
3. Mutations in UCH-L1 (autosomal recessive form)
4. Mutations in DJ-1 (autosomal recessive form)
Berry Aneurysm
Berry Aneurysm
Most common locations of Berry Aneurysms:
· Anterior cerebral artery (anterior communicating artery)
· Middle cerebral artery
· Internal carotid artery
Associated systemic conditions for Berry Aneurysms:
· ADPCKD
· Ehlers-Danlos syndrome (type IV)
· Neurofibromatosis type 1
· Marfan syndrome
· Coarctation of aorta
· Fibromuscular dysplasia of extracranial arteries
Predisposing factors for Berry Aneurysms:
- Cigarette smoking and hypertension are
Berry Aneurysm Gross Features
Unruptured aneurysms are a thin-walled arterial outpouchings at branch points of the circle of Willis or a major vessel just beyond. Measure 2-3 mm and are shiny, bright red surface with thin, translucent wall. Atheromatous plaques, thrombosis, or calcification may be found in wall or lumen of aneurysm. Brownish discolouration of brain/meninges indicates previous hemorrhage. Rupture occurs at apex of sac with extravasation of blood to subarachnoid space, substance of brain, or both.
Histological Features of Berry Aneurysms:
Arterial wall adjacent to aneurysm shows intimal thickening and attenuation of media as it approaches the neck of the aneurysm. At the neck of the aneurysm the muscular wall and intimal elastic lamina stop short and are absent from the aneurysmal wall itself. The sac is made up of thickened, hyalinised intima. The adventitia covering the sac is continuous with that of the parent artery
References:
Robbins Basic Pathology 7th ed, edited by Vinay Kumar, Ramzi S. Cotran, and Stanley J. Robbins, 873 pp, Philadelphia, Pa, Sounders, 2003.
Posted in Brain, Vascular
Tagged , aneurysm, aneurysms, berry, berry aneurysm, cigarette, hypertension, marfan syndrome, smoking
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