Neurodegenerative diseases

Neurodegenerative diseases is a big part of neuropathology.

Overview

• Neurodegenerative disease = essentially progressive and selective neuron loss.
• Clinically, they are not unique, e.g. dementia can be caused by several diseases (with different molecular etiologies).
  • Each syndrome (e.g. dementia, parkinsonism, ataxia) has a most common etiology and a DDx.
• They are defined by molecular pathology.^[1]
  • The diseases are due to the accumulation of abnormal protein.
    • The amino acid sequence of the protein may be completely normal. The problem may just be folding/protein conformation.

Molecular schema of neurodegenerative disorders:^[1]

Neurodegenerative disorders

Amyloidoses

Tauopathies

α-synucleinopathies

TDP-43

Common diseases

Amyloidoses:

• Alzheimer disease (Abeta).
• Creutzfeldt-Jakob disease (PrP).

Taupathies:

• Progressive supranuclear palsy.
• Pick's disease.

Synucleinopathies:^[2]

• Parkinson disease.
• Dementia with Lewy bodies.
• Multiple system atrophy.

TDP-43 proteinopathies:

• Amyotrophic alteral sclerosis.
• Frontotemporal lobar degeneration with ubiquitinated inclusions.

Table

Disease/pathology/clinical correlation based on Dickson:^[1]

Disease	Mutated protein	Distribution	Clinical	Histology	Image
Alzheimer disease	Abeta (mutated APP)	corticolimbic, usu. spares occipital	dementia	plaques, neurofibrillary tangles ???	Image?
Creutzfeldt-Jakob disease	PrPres (mutated PrP)	cortical & basal ganglia	dementia (rapid progression), movement disorder	cytoplasmic vacuolization	Image?
Progressive supranuclear palsy	tau 4R	basal ganglia, brainstem	parkinsonism	globose neurofibrillary tangles in neurons, coiled bodies in oligodendrocytes	Image?
Pick disease	tau 3R	corticolimbic	dementia + focal cortical syndrome	Pick body ???	Image?
Parkinson disease	alpha-synuclein	brainstem	parkinsonism	Lewy bodies	Image?
Dementia with Lewy bodies	alpha-synuclein	corticolimbic, brainstem	dementia + parkinsonism	Lewy bodies	Image?
Multiple system atrophy	alpha-synuclein	basal ganglia, brainstem, cerebellum	parkinsonism, ataxia	cytoplasmic inclusion in oligodendrocytes[3]	Image
Amyotrophic lateral sclerosis (ALS)	TDP-43	motor neurons	spasticity, weakness	histology?	Image
Frontotemporal lobar degeneration with ubiquitinated inclusions	TDP-43	cortex, basal ganglia	dementia, focal cortical syndromes	histology?	Image?

IHC

Alpha-synuclein

Look for:

• Lewy bodies (seen in Parkinson's d., Dementia with Lewy bodies) = round cytoplasmic eosinophilic body +/- pale halo.

Tau

• AT8 = stains phosphorylated tau.^[4]
  • AT = anti-tau.
  • Stains tau 4R and tau 3R.^[5]

TDP-43

• May accumulate due to a progranulin mutation.

Microscopic

• TDP-43 - normally in the nucleus.
  • Pathologic: Micrograph (label B) - neurites, skein-like formations (ama-assn.org)^[6]
    • Fibrillar or skein-like formations = cytoplasmic staining.
      • "Skein" = yarn or thread wound on a reel or flock of birds in flight.^[7]
    • Neurites = "squiggly appearance"; "worm-like appearance".

Ubiquitin

• Marks proteins for recycling.

Microscopic

• p62; poli-ubiquitin-binding protein p62.^[4]

Look for:

• Lewy bodies. (???)

Clinical perspective

General (mostly useless) DDx

• Alzheimer's dementia - most common.
• Vascular.
  • Multi-infarct dementia.
• Parkinson's associated dementia.
• Lewy body dementia.
• Alcohol-related dementia.
• Fronto-temporal dementia (Pick disease).
• Multisystem atrophy.

Mnemonic

Mnemonic VITAMIN D VEST:^[8]

• Vitamin deficiency (B12, folate, thiamine).
• Infection (HIV).
• Trauma.
• Anoxia.
• Metabolic (Diabetes).
• Intracranial tumour.
• Normal pressure hydrocephalus.
• Degenerative (Alzheimer's, Huntington's, CJD).
• Vascular.
• Endocrine.
• Space occupying lesion (chronic subdural hematoma).
• Toxins (alcohol).

Functional anatomy of dementia

• Hippocampus (essential for forming new memories).
• Frontal lobe (essential for retrieval of memories).

Alzheimer disease

General

• Onset: episodic memory loss.
• Diagnosis is clinical & pathologic.
  • Pathologic finding alone are not diagnostic.

Gross

Features:

• Temporal atrophy, esp. hippocampus.
• Dilation of:
  • Lateral ventricles.
  • Third ventricle.

Gross/microscopic - disease spread by NF tangles (staging):^[9]

• Alzheimer "spreads" in a reproducible pattern:
  • Stage I-II: entorhinal cortex.
  • Stage III-IV: inferior aspect of brain.
  • Stage V-VI: limbic system.

Microscopic

Features:

1. Neurofibrillary tangles.
   • Consists of tau.
   • Location: hippocampus, cerebral cortex, hypothalamus.
   • Images: tangles - schematic (pakmed.net)^[10], tangle (washington.edu).^[11]
2. Senile plaques.
   • Consists of two components:
     1. Centre - radiates.
        • Consists of Abeta amyloid
     2. Neurites - swollen axons.
   • Considered to be more specific for Alzheimer's than NF tangles.
   • There is a staging system for plaques I (mild), II (moderate), III (severe).
   • Image: Senile plaques (utah.edu).^[12]

Notes:

• Abeta amyloid:
  • Derived from amyloid precursor protein (APP).
    • APP:
      • Rapid axonal transport - useful as a marker of axonal injury.
      • Function currently not known.
• Tau:
  • Important in microtubule assembly.

Lewy body diseases

DDx:

• Parkinson's disease.
• Dementia with Lewy bodies.

Etiology:

• Alpha-synuclein.

Clinical features of Dementia with Lewy bodies:

• Parkinsonian features.
• Hallucinations (visual).
• Progressive cognitive decline with fluctuations.

Multiple system atrophy

General

Clinical findings variable:

• Parkinsonism (stiatonigral degeneration).
• Ataxia (olivo-panto-cerebellar degeneration).

Microscopic

Features:

• Alpha-synuclein-rich glial cytoplasmic inclusions (finding at autopsy).^[13]
  • Inclusions in oligodendrocytes.^[14]

Progressive supranuclear palsy

General

• AKA Steele-Richardson-Olszewski syndrome.
• Commonly abbreviated PSP.
• Diagnosis: clinical.^[15]

Microscopic

Features:^[1][15][16]

• Globose neurofibrillary tangles in neurons.
• Coiled bodies in oligodendrocytes.
  • Wire coil-like structure around the nucleus.
• Tufted astrocytes.
  • Near impossible to see without IHC - specifically AT8.
  • Cellular processes filled with crap.
  • Star-like appearance; looks like a road network where all the roads lead to one place (Parisian star).
• Grumose degeneration of the cerebellar dentate nucleus.
  • Granular eosinophilic material adjacent to nuclei; once thought to be pathognomonic for PSP.^[17][18]

Huntington disease

General

• Autosomal dominant inheritance.
• Mutation: unstable CAG repeat.^[19]

Gross

• Missing caudate.^[20]

Image: Huntington's disease (ouhsc.edu).

Binswanger's disease

General

• Multi-infarct dementia affecting subcortical white matter.
• Waste-basket diagnosis; diagnosed if CADASIL and amyloidosis have been excluded.
• Diagnosis has been controversial -- most with this entity (in the past) were diagnosed with Alzheimer's disease.

Microscopic

Features:

• Subcortical lesions that replace the myelin consisting of macrophages.

Amyotrophic lateral sclerosis

General

• Abbreviated ALS.
• Weakness.

Prion diseases

Etiology:^[21]

• Misfolded cell-surface protein called PrP(C).

Includes:^[21]

• Creutzfeldt-Jakob disease (CJD).
• Sporadic fatal insomnia (sFI).

Creutzfeldt-Jakob disease

General

• Commonly abbreviated as CJD.
• Rare.
• Incurable disease.

• Usually diagnosed clinically.
  • Characteristic findings:
    • Very rapid decline (3-4 months).
    • Characteristic (cortex findings on) neuroradiology.

Variant Creutzfeldt-Jakob disease (vCJD)

• Associated with bovine spongiform encephalopathy.
• Should sample: spleen, lymph nodes, tonsils.^[22]

Microscopic

Features:

• Spongy appearance (cytoplasmic vacuolization^[23]).

Images:

• CJD (WC).
• vCJD - IHC (WC).

See also

• Neuropathology.
• Neurohistology.

References