Difference between revisions of "Neurodegenerative diseases"

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'''Neurodegenerative diseases''' is a big part of [[neuropathology]].   
'''Neurodegenerative diseases''' is a big part of [[neuropathology]].  It includes some discussion of '''dementia'''.


==Overview==
=Overview=
*They are essentially progressive and selective neuron loss.   
*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).
*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.<ref name=pmid19918325>{{cite journal |author=Dickson DW |title=Neuropathology of non-Alzheimer degenerative disorders |journal=Int J Clin Exp Pathol |volume=3 |issue=1 |pages=1–23 |year=2009 |pmid=19918325 |pmc=2776269 |doi= |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2776269/?tool=pubmed}}</ref>
*They are defined by molecular pathology.<ref name=pmid19918325>{{cite journal |author=Dickson DW |title=Neuropathology of non-Alzheimer degenerative disorders |journal=Int J Clin Exp Pathol |volume=3 |issue=1 |pages=1–23 |year=2009 |pmid=19918325 |pmc=2776269 |doi= |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2776269/?tool=pubmed}}</ref>
**The diseases are due to the accumulation of abnormal protein.
**The diseases are due to the accumulation of abnormal protein.
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{{familytree/start}}                       
{{familytree/start}}                       
{{familytree  | | | | | | | A01 | | | | | | | | A01=Neurodegenerative<br>disorders}}
{{familytree  | | | | | | | A01 | | | | | | | | A01=Neurodegenerative<br>disorders}}
{{familytree  | |,|-|-|-|v|-|^|-|v|-|-|-|.| | |}}
{{familytree  | |,|-|-|-|v|-|^|-|v|-|-|-|v|-|-|-|.| | |}}
{{familytree  | B01 | | B02 | | B03 | | B04 | |B01=Amyloidoses|B02=Tauopathies|B03=α-synucleinopathies|B04=TDP-43}}
{{familytree  | B01 | | B02 | | B03 | | B04 | | B05 || B01=Amyloidoses|B02=Tauopathies|B03=α-synucleinopathies|B04=TDP-43|B05=FUS/EWS/TAF15}}
{{familytree/end}}
{{familytree/end}}


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[[Amyloid]]oses:
[[Amyloid]]oses:
*Alzheimer disease (Abeta).
*Alzheimer disease (Abeta).
*Creutzfeldt-Jakob disease (PrP).


Taupathies:
'Pure' tauopathies:
*Progressive supranuclear palsy.
*[[Progressive supranuclear palsy]].
*Pick's disease.
*[[Pick's disease]].
*Corticobasal degeneration.
*FTDP-17.
*[[Dementia pugilistica]].


Synucleinopathies:<ref name=pmid18855701>{{Cite journal  | last1 = Uversky | first1 = VN. | title = Alpha-synuclein misfolding and neurodegenerative diseases. | journal = Curr Protein Pept Sci | volume = 9 | issue = 5 | pages = 507-40 | month = Oct | year = 2008 | doi =  | PMID = 18855701 }}</ref>
Synucleinopathies:<ref name=pmid18855701>{{Cite journal  | last1 = Uversky | first1 = VN. | title = Alpha-synuclein misfolding and neurodegenerative diseases. | journal = Curr Protein Pept Sci | volume = 9 | issue = 5 | pages = 507-40 | month = Oct | year = 2008 | doi =  | PMID = 18855701 }}</ref>
*Parkinson disease.
*[[Parkinson disease]].
*Dementia with Lewy bodies.
*Dementia with [[Lewy bodies]].
*Multiple system atrophy.
*[[Multiple system atrophy]].


TDP-43 proteinopathies:
TDP-43 proteinopathies:
*Amyotrophic alteral sclerosis.
*[[Amyotrophic lateral sclerosis]].
*Frontotemporal lobar degeneration with ubiquitinated inclusions.
*Frontotemporal lobar degeneration with TDP-43 (FTLD-TDP).
 
FET proteinopathies:
*Basophilic inclusion body disease (BIBD).
*Neuronal intermediate filament inclusion disease (NIFID).
*Atypical frontotemporal lobar degeneration with ubiquitin-positive inclusions (atypical FTLD-U).
 
Prionopathies:
*Creutzfeldt-Jakob disease (PrP).
'''Note:''' Some people consider α-synuclein as a prion-like protein.<ref>{{Cite journal  | last1 = Watts | first1 = JC. | title = Calling α-synuclein a prion is scientifically justifiable. | journal = Acta Neuropathol | volume = 138 | issue = 4 | pages = 505-508 | month = Oct | year = 2019 | doi = 10.1007/s00401-019-02058-0 | PMID = 31407029 }}</ref>


====Table====
====Table====
Disease/pathology/clinical correlation based on ''Dickson'':<ref name=pmid19918325>{{cite journal |author=Dickson DW |title=Neuropathology of non-Alzheimer degenerative disorders |journal=Int J Clin Exp Pathol |volume=3 |issue=1 |pages=1–23 |year=2009 |pmid=19918325 |pmc=2776269 |doi= |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2776269/?tool=pubmed}}</ref>
Disease/pathology/clinical correlation based on ''Dickson'':<ref name=pmid19918325>{{cite journal |author=Dickson DW |title=Neuropathology of non-Alzheimer degenerative disorders |journal=Int J Clin Exp Pathol |volume=3 |issue=1 |pages=1–23 |year=2009 |pmid=19918325 |pmc=2776269 |doi= |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2776269/?tool=pubmed}}</ref>
{| class="wikitable sortable" style="margin-left:auto;margin-right:auto"
{| class="wikitable sortable" style="margin-left:auto;margin-right:auto"
| '''Disease'''
! Disease
| '''Mutated protein'''
! Deposited protein
| '''Distribution'''
! Distribution
| '''Clinical'''
! Clinical
| '''Histology'''
! Histology
| '''Image'''
! Image
|-
|-
| Alzheimer disease
| [[Alzheimer disease]]
| Abeta (mutated ''APP'')
| Abeta (mutated ''APP'')
| corticolimbic, usu. <br>spares occipital
| corticolimbic, usu. <br>spares occipital
| dementia  
| dementia  
| histology?
| plaques, neurofibrillary tangles
| Image?
| [http://en.wikipedia.org/wiki/File:Cerebral_amyloid_angiopathy_-2a-_amyloid_beta_-_high_mag.jpg]
|-
|-
| Creutzfeldt-Jakob disease
| [[Creutzfeldt-Jakob disease]]
| PrP<sup>res</sup> (mutated PrP)
| PrP<sup>res</sup> (mutated PrP)
| cortical & basal ganglia
| cortical & basal ganglia
| dementia (rapid progression), <br>movement disorder  
| dementia (rapid progression), <br>movement disorder  
| plaques, neurofibrillary tangles ???
| cytoplasmic vacuolization, PrP+ve plaques, Kuru plaques (MV2 variant)
| Image?
| [http://en.wikipedia.org/wiki/File:SpongiformChangeCJD.jpg]
|-
| Progressive supranuclear palsy
| tau 4R
| basal ganglia, brainstem
| parkinsonism
| histology?
| Image?
|-
|-
| Pick disease
| [[Parkinson disease]]
| tau 3R
| corticolimbic
| dementia + focal <br>cortical syndrome
| Pick body ???
| Image?
|-
| Parkinson disease
| alpha-synuclein
| alpha-synuclein
| brainstem
| brainstem
| parkinsonism  
| parkinsonism  
| histology?
| Lewy bodies in substantia nigra and locus coeruleus
| Image?
| [http://firstaidteam.com/usmlerximages/v/USMLERxLewy+bodies.gif.html] [https://de.wikipedia.org/wiki/Datei:LewyBodies_small.JPG]
|-
|-
| Dementia with <br>Lewy bodies
| [[Dementia with Lewy bodies|Dementia with <br>Lewy bodies]]
| alpha-synuclein
| alpha-synuclein
| corticolimbic, brainstem
| corticolimbic, brainstem
| dementia + parkinsonism
| dementia + parkinsonism
| histology?
| Lewy bodies brainstem and cortical, tangles
| Image?
| [http://firstaidteam.com/usmlerximages/v/USMLERxLewy+bodies.gif.html] [https://commons.wikimedia.org/wiki/File:DLB_frontal_lewy_bodies_HE.jpg]
|-
|-
| Multiple system atrophy
| [[Multiple system atrophy]]
| alpha-synuclein
| alpha-synuclein
| basal ganglia, brainstem, cerebellum
| basal ganglia, brainstem, cerebellum
| parkinsonism, ataxia  
| parkinsonism, ataxia  
| histology?
| Papp-Lantos inclusions (cytoplasmic deposits in oligodendrocytes)<ref>MUN. 15 November 2010.</ref>
| Image
| [https://commons.wikimedia.org/wiki/File:MSA_Gallays_Papp_Lantos_inclusions.jpg]
|-
|-
| Amyotrophic lateral <br>sclerosis (ALS)
| [[Amyotrophic lateral sclerosis|Amyotrophic lateral <br>sclerosis (ALS)]]
| TDP-43
| [[TDP-43]]
| motor neurons
| motor neurons
| spasticity, weakness
| spasticity, weakness
| histology?
| motor neuron loss, TDP-43+ve, TAF15-ve, EWS-ve inclusions in motor neurons
| Image
| [https://commons.wikimedia.org/wiki/File:Als_inclusions.png]
|-  
|-  
| Frontotemporal lobar <br>degeneration with <br>ubiquitinated inclusions
| Frontotemporal lobar <br>degeneration with TDP-43 (FTLD-TDP)
| TDP-43
| [[TDP-43]]
| cortex, basal ganglia
| cortex, basal ganglia
| dementia, focal cortical syndromes
| dementia, focal cortical syndromes
| histology?
| histology depends on (type 1-4), ubiquitin and [[TDP-43]]+ve, tau and FUS-ve
| Image?
| [https://commons.wikimedia.org/wiki/File:FTLD_TSP43_hippocampus.jpg]
|-
| Frontotemporal lobar <br>degeneration with FET (FTLD-FET)
| FUS/EWS/TAF15
| cortex, medulla, hippocampus, and motor cells of the spinal cord
| dementia, cases classified as aFTLD-U, NIFID and BIBD
| FUS+ve, TAF15+ve, EWS+ve cytoplasmic & intranuclear inclusions, neuritic threads
| [http://brain.oxfordjournals.org/content/brain/134/9/2595/F1.medium.gif]
|-
|-
| [[Progressive supranuclear palsy]] (FTLD-tau)
| tau 4R
| basal ganglia, brainstem
| atypical parkinsonism with early gait instability, falls, and supranuclear gaze palsy
| tau-positive globose neurofibrillary tangles <br>in neurons, tufted astrocytes, coiled bodies <br>in oligodendrocytes
| [https://commons.wikimedia.org/wiki/File:PSP_Tau_tufted_astrocyte.jpg]
|-
| [[Pick disease]] (FTLD-tau)
| tau 3R
| corticolimbic
| dementia + focal <br>cortical syndrome
| Intraneuronal argyrophilic inclusions (Pick body)
| [http://frontalcortex.com/gallery/pics/gliageek_PBtau.jpg]
|-
| Corticobasal degeneration (CBD) (FTLD-tau)
| tau 4R
| cortical, basal ganglia
| dementia + movement disorder (Parkinson-plus syndrome)
| ballooned neurons, astrocytic plaques, pretangles in basal nucleus
| [http://webeye.ophth.uiowa.edu/eyeforum/cases-i/case155/4-Progressive-Supranuclear-Palsy-histology.jpg]
|-
| Argryophilic grain disease (AGD) (FTLD-tau)
| tau 4R
| medial temporal lobe, limbic structures
| late-onset amnestic syndrome
| Argyrophilic grains (also found unspecific in elederly)
| [http://de.wikipedia.org/wiki/Silberkornkrankheit#/media/File:AGD_gallays.jpg]
|- <!--
|- <!--
| Disease
| Disease
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|}
|}


==IHC==
=Immunohistochemistry=
*AT-8 = stains phosphorylated tau.<ref name=pmid19946779>{{cite journal |author=Seelaar H, Klijnsma KY, de Koning I, ''et al.'' |title=Frequency of ubiquitin and FUS-positive, TDP-43-negative frontotemporal lobar degeneration |journal=J. Neurol. |volume=257 |issue=5 |pages=747–53 |year=2010 |month=May |pmid=19946779 |pmc=2864899 |doi=10.1007/s00415-009-5404-z |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2864899/}}</ref>
===Alpha-synuclein===
*p62; poli-ubiquitin-binding protein p62.<ref name=pmid19946779/>
Look for:
*Lewy bodies (seen in Parkinson's Disease (PD), Dementia with Lewy bodies (DLB)) = round cytoplasmic eosinophilic body +/- pale halo.
*Lewy neurites(seen in [[PD]] and [[DLB]]) = abnormal neurites with filaments similar to those found in Lewy bodies.
*Glial cytoplasmatic inclusions (Papp-Lantos bodies) seen in mutisystem atrophy (MSA).
*Beta amyloid in vessels seen in cerebral amyloid angiopathy (CAA).
 
===Tau===
*AT8 = stains phosphorylated tau.<ref name=pmid19946779>{{cite journal |author=Seelaar H, Klijnsma KY, de Koning I, ''et al.'' |title=Frequency of ubiquitin and FUS-positive, [[TDP-43]]-negative frontotemporal lobar degeneration |journal=J. Neurol. |volume=257 |issue=5 |pages=747–53 |year=2010 |month=May |pmid=19946779 |pmc=2864899 |doi=10.1007/s00415-009-5404-z |url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2864899/}}</ref>
**''AT'' = anti-tau.
**Stains tau 4R and tau 3R.<ref>{{cite journal |author=Kumaran R, Kingsbury A, Coulter I, ''et al.'' |title=DJ-1 (PARK7) is associated with 3R and 4R tau neuronal and glial inclusions in neurodegenerative disorders |journal=Neurobiol. Dis. |volume=28 |issue=1 |pages=122–32 |year=2007 |month=October |pmid=17719794 |doi=10.1016/j.nbd.2007.07.012 |url=}}</ref>
 
===TDP-43===
*May accumulate due to a ''progranulin mutation''.
 
====Microscopic====
*TDP-43 - normally in the nucleus.
*TDP-43 - normally in the nucleus.
**Pathologic: [http://archneur.ama-assn.org/cgi/content/full/65/5/636/NOC70108F2 Micrograph (label B) - neurites, skein-like formations (ama-assn.org)]<ref>{{cite journal |author=Geser F, Brandmeir NJ, Kwong LK, ''et al.'' |title=Evidence of multisystem disorder in whole-brain map of pathological TDP-43 in amyotrophic lateral sclerosis |journal=Arch. Neurol. |volume=65 |issue=5 |pages=636–41 |year=2008 |month=May |pmid=18474740 |doi=10.1001/archneur.65.5.636 |url=}}</ref>
**Pathologic: [http://archneur.ama-assn.org/cgi/content/full/65/5/636/NOC70108F2 Micrograph (label B) - neurites, skein-like formations (ama-assn.org)]<ref>{{cite journal |author=Geser F, Brandmeir NJ, Kwong LK, ''et al.'' |title=Evidence of multisystem disorder in whole-brain map of pathological TDP-43 in amyotrophic lateral sclerosis |journal=Arch. Neurol. |volume=65 |issue=5 |pages=636–41 |year=2008 |month=May |pmid=18474740 |doi=10.1001/archneur.65.5.636 |url=}}</ref>
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***''Neurites'' = "squiggly appearance"; "worm-like appearance".
***''Neurites'' = "squiggly appearance"; "worm-like appearance".


==Clinical perspective (becoming obsolete)==
===Ubiquitin===
===General (mostly useless) DDx===
*Marks proteins for recycling.
*Alzheimer's dementia - most common.
*Stains Barr bodies in hippocampal granule cells<ref> {{Cite journal  | last1 = Gelpi | first1 = E. | title = Clinical Neuropathology teaching case 3-2015: female or male brain? Anti-ubiquitin visualizes Barr bodies in hippocampal granule cells which allows the determination of gender in human brains. | journal = Clin Neuropathol | volume = 34 | issue = 3 | pages = 115-6 | month =  | year =  | doi =  | PMID = 25909954 }}</ref>
 
 
===p62===
*p62; poli-ubiquitin-binding protein p62.<ref name=pmid19946779/>
 
===Microscopic===
Look for:
* Lewy bodies and extracellular pigment in neuromelanin-containing nuclei (SN, LC, DVN) -> PD.
* Spongiform vacuolation in the neuropil (seen in Prion disease and FTLD-TDP).
* Neurofibrillar tangles (pyramidal layer of dentate gyrus).
* Granulovacuolar degeneration (granules within cytoplasmic vacuoles, mainly in the hippocampal pyramidal neurons, seen in AD).
* Cores of amyloid plaqyes.
* Cotton wool plaques (seen in familiar AD).
* Pick cells (balloned neurons in frontal cortex).
* Pick bodies (granular layer of dentate gyrus).
* Extensive astrogliosis (striatonigral degeneration, hepatic encephalopathy).
* Corpora amylacea in the cornu ammonis may be increased in neurodegenerative diseases. <ref>{{Cite journal  | last1 = Kovacs | first1 = GG. | last2 = Risser | first2 = D. | title = Clinical Neuropathology image 6-2014: Corpora amylacea replacing cornu ammonis (CACA). | journal = Clin Neuropathol | volume = 33 | issue = 6 | pages = 378-9 | month =  | year =  | doi =  | PMID = 25343241 }}</ref>
<gallery>
File:213-09-11-Congo Red Lewy body.tif|Lewy body
File:Amyloid plaques alzheimer disease HE stain.jpg|Cotton wool plaques
File:Neurofibrillary tangles in the Hippocampus of an old person with Alzheimer-related pathology, HE 3.JPG|Neurofibrillary tangles
File:SpongiformChangeCJD.jpg | Spongiform vacuolation
</gallery>
 
=Clinical perspective=
*Correlations between clinical signs and molecular can be poor.
**Example: The MAPT A152T gene mutation may cause clinical symptoms matching AD, [[Neurodegenerative diseases#Corticobasal degeneration|CBD]], [[Neurodegenerative diseases#Progressive supranuclear palys|PSP]] and  [[Neurodegenerative diseases#Lewy body disease|LBD]].<ref>{{Cite journal  | last1 = Coppola | first1 = G. | last2 = Chinnathambi | first2 = S. | last3 = Lee | first3 = JJ. | last4 = Dombroski | first4 = BA. | last5 = Baker | first5 = MC. | last6 = Soto-Ortolaza | first6 = AI. | last7 = Lee | first7 = SE. | last8 = Klein | first8 = E. | last9 = Huang | first9 = AY. | title = Evidence for a role of the rare p.A152T variant in MAPT in increasing the risk for FTD-spectrum and Alzheimer's diseases. | journal = Hum Mol Genet | volume = 21 | issue = 15 | pages = 3500-12 | month = Aug | year = 2012 | doi = 10.1093/hmg/dds161 | PMID = 22556362 }}</ref>
 
===Dementia general (mostly useless) DDx===
*[[Alzheimer's disease|Alzheimer's]] dementia - most common.
*Vascular.
*Vascular.
**Multi-infarct dementia.
**Multi-infarct dementia.
*Parkinson's associated dementia.
*Parkinson's associated dementia.
*Lewy body dementia.
*Lewy body dementia.
*Alcohol-related dementia.
*[[Alcohol]]-related dementia.
*Fronto-temporal dementia (Pick disease).
*Fronto-temporal dementia (Pick disease).
*Multisystem atrophy.
*Multisystem atrophy.


===Mnemonic===
====Mnemonic====
Mnemonic ''VITAMIN D VEST'':<ref>TN06 PS19</ref>
Dementia mnemonic ''VITAMIN D VEST'':<ref name=Ref_TN2006_PS19>{{Ref TN2006| PS19}}</ref>
*Vitamin deficiency (B12, folate, thiamine).
*Vitamin deficiency (B12, folate, thiamine).
*Infection (HIV).
*Infection (HIV).
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*Toxins (alcohol).
*Toxins (alcohol).


===Functional anatomy of dementia===
====Functional anatomy of dementia====
*Hippocampus (essential for forming new memories).
*[[Hippocampus]] (essential for forming new memories).
*Frontal lobe (essential for retrieval of memories).
*Frontal lobe (essential for retrieval of memories).


==Lewy body diseases==
===Parkinsonism causes===
DDx:
*Parkinson's disease <ref name=pmid17390256>{{Cite journal  | last1 = Tuite | first1 = PJ. | last2 = Krawczewski | first2 = K. | title = Parkinsonism: a review-of-systems approach to diagnosis. | journal = Semin Neurol | volume = 27 | issue = 2 | pages = 113-22 | month = Apr | year = 2007 | doi = 10.1055/s-2007-971174 | PMID = 17390256 }}</ref>
*Parkinson's disease.
*[[Dementia with Lewy bodies]].
*Dementia with Lewy bodies.
*[[Multiple system atrophy]] (MSA).<ref name=pmid22074330>{{Cite journal  | last1 = Ahmed | first1 = Z. | last2 = Asi | first2 = YT. | last3 = Sailer | first3 = A. | last4 = Lees | first4 = AJ. | last5 = Houlden | first5 = H. | last6 = Revesz | first6 = T. | last7 = Holton | first7 = JL. | title = Review: The neuropathology, pathophysiology and genetics of multiple system atrophy. | journal = Neuropathol Appl Neurobiol | volume =  | issue =  | pages =  | month = Nov | year = 2011 | doi = 10.1111/j.1365-2990.2011.01234.x | PMID = 22074330 }}</ref>
*[[Progressive supranuclear palsy]] (PSP).<ref name=pmid22228724>{{Cite journal  | last1 = Bertram | first1 = K. | last2 = Williams | first2 = DR. | title = Visual hallucinations in the differential diagnosis of parkinsonism. | journal = J Neurol Neurosurg Psychiatry | volume = 83 | issue = 4 | pages = 448-52 | month = Apr | year = 2012 | doi = 10.1136/jnnp-2011-300980 | PMID = 22228724 }}</ref>
*Drug induced (valproic acid, MPTP).<ref name=pmid21993183>{{Cite journal  | last1 = Mahmoud | first1 = F. | last2 = Tampi | first2 = RR. | title = Valproic Acid-Induced Parkinsonism in the Elderly: A Comprehensive Review of the Literature. | journal = Am J Geriatr Pharmacother | volume =  | issue =  | pages =  | month = Oct | year = 2011 | doi = 10.1016/j.amjopharm.2011.09.002 | PMID = 21993183 }}</ref><ref name=pmid1815982> {{Cite journal  | last1 = Gerlach | first1 = M. | last2 = Riederer | first2 = P. | last3 = Przuntek | first3 = H. | last4 = Youdim | first4 = MB. | title = MPTP mechanisms of neurotoxicity and their implications for Parkinson's disease. | journal = Eur J Pharmacol | volume = 208 | issue = 4 | pages = 273-86 | month = Dec | year = 1991 | doi =  | PMID = 1815982 }}</ref>
* Vascular. <ref name=pmid25917706>{{Cite journal  | last1 = Korczyn | first1 = AD. | title = Vascular parkinsonism-characteristics, pathogenesis and treatment. | journal = Nat Rev Neurol | volume =  | issue =  | pages =  | month = Apr | year = 2015 | doi = 10.1038/nrneurol.2015.61 | PMID = 25917706 }}</ref>
* Postencephalitic. <ref name=pmid20629120>{{Cite journal  | last1 = Vilensky | first1 = JA. | last2 = Gilman | first2 = S. | last3 = McCall | first3 = S. | title = A historical analysis of the relationship between encephalitis lethargica and postencephalitic parkinsonism: a complex rather than a direct relationship. | journal = Mov Disord | volume = 25 | issue = 9 | pages = 1116-23 | month = Jul | year = 2010 | doi = 10.1002/mds.22908 | PMID = 20629120 }}</ref>
* Tramuatic (Dementia pugilistica).<ref name=pmid24398724>{{Cite journal  | last1 = Chauhan | first1 = NB. | title = Chronic neurodegenerative consequences of traumatic brain injury. | journal = Restor Neurol Neurosci | volume = 32 | issue = 2 | pages = 337-65 | month =  | year = 2014 | doi = 10.3233/RNN-130354 | PMID = 24398724 }}</ref>
 
=Amyloidoses=
==Alzheimer disease==
===General===
*Onset: episodic memory loss.
*Diagnosis is clinical & pathologic.
**Pathologic finding alone are not diagnostic.
**Onset, rate of progression and the development of pathology are highly variable.
*Defined by:
**Pathological accumulation of amyloid β (Aβ) into extracellular plaques.
**Abnormally phosphorylated tau that accumulates intraneuronally forming neurofibrillary tangles (NFTs).
**Clinicopathological correlation better for NFT than for Aβ.<ref>{{Cite journal  | last1 = Nelson | first1 = PT. | last2 = Alafuzoff | first2 = I. | last3 = Bigio | first3 = EH. | last4 = Bouras | first4 = C. | last5 = Braak | first5 = H. | last6 = Cairns | first6 = NJ. | last7 = Castellani | first7 = RJ. | last8 = Crain | first8 = BJ. | last9 = Davies | first9 = P. | title = Correlation of Alzheimer disease neuropathologic changes with cognitive status: a review of the literature. | journal = J Neuropathol Exp Neurol | volume = 71 | issue = 5 | pages = 362-81 | month = May | year = 2012 | doi = 10.1097/NEN.0b013e31825018f7 | PMID = 22487856 }}</ref>
*Seen in conjunction with vascular amyloid deposition; see ''[[cerebral amyloid angiopathy]]''.
*Evidence of possible iatrogenic transmission by cadaver-sourced growth hormone batches.<ref>{{Cite journal  | last1 = Duyckaerts | first1 = C. | last2 = Sazdovitch | first2 = V. | last3 = Ando | first3 = K. | last4 = Seilhean | first4 = D. | last5 = Privat | first5 = N. | last6 = Yilmaz | first6 = Z. | last7 = Peckeu | first7 = L. | last8 = Amar | first8 = E. | last9 = Comoy | first9 = E. | title = Neuropathology of iatrogenic Creutzfeldt-Jakob disease and immunoassay of French cadaver-sourced growth hormone batches suggest possible transmission of tauopathy and long incubation periods for the transmission of Abeta pathology. | journal = Acta Neuropathol | volume = 135 | issue = 2 | pages = 201-212 | month = Feb | year = 2018 | doi = 10.1007/s00401-017-1791-x | PMID = 29209767 }}</ref><ref>{{Cite journal  | last1 = Jaunmuktane | first1 = Z. | last2 = Mead | first2 = S. | last3 = Ellis | first3 = M. | last4 = Wadsworth | first4 = JD. | last5 = Nicoll | first5 = AJ. | last6 = Kenny | first6 = J. | last7 = Launchbury | first7 = F. | last8 = Linehan | first8 = J. | last9 = Richard-Loendt | first9 = A. | title = Evidence for human transmission of amyloid-β pathology and cerebral amyloid angiopathy. | journal = Nature | volume = 525 | issue = 7568 | pages = 247-50 | month = Sep | year = 2015 | doi = 10.1038/nature15369 | PMID = 26354483 }}</ref>
 
 
 
 
 
====Genetics====
Genes associated with Alzheimer disease:<ref>{{Ref PCPBoD8|674-5}}</ref>
*Amyloid precursor protein (APP).
**On chromosome 21 - may explain why [[Trisomy 21]] (Down syndrome) increases the risk of Alzheimer disease.<ref name=pmid19269132>{{Cite journal  | last1 = Nieuwenhuis-Mark | first1 = RE. | title = Diagnosing Alzheimer's dementia in Down syndrome: problems and possible solutions. | journal = Res Dev Disabil | volume = 30 | issue = 5 | pages = 827-38 | month =  | year =  | doi = 10.1016/j.ridd.2009.01.010 | PMID = 19269132 }}</ref>
*Presenilin 1 (PSEN1).<ref name=omim104311>{{OMIM|104311}}</ref>
*Presenilin 2 (PSEN2).<ref name=omim600759>{{OMIM|600759}}</ref>
*Apolipoprotein E (APOE)<ref name=omim107741>{{OMIM|107741}}</ref> - specifically the ''epsilon-4'' allele.
 
===Gross===
Features:
*Temporal atrophy, esp. hippocampus.
*Dilation of:
**Lateral ventricles.
**Third ventricle.
 
Gross/microscopic - disease spread by NF tangles (staging):<ref name=pmid8307060>{{cite journal |author=Braak H, Braak E, Bohl J |title=Staging of Alzheimer-related cortical destruction |journal=Eur. Neurol. |volume=33 |issue=6 |pages=403–8 |year=1993 |pmid=8307060 |doi= |url=}}</ref>
*Alzheimer "spreads" in a reproducible pattern:
**Stage I-II: entorhinal cortex.
**Stage III-IV: inferior aspect of brain.
**Stage V-VI: limbic system.
 
Minimal sampling:
* Frontal, parietal & temporal lobe
* Hippocampus and entorhinal cortex
Additional sampling:
* Basal ganglia
* Cerebellum
* Midbrain (including substantia nigra)
* Occipital cortex
 
====Images====
<gallery>
Image:Alzheimers_brain.jpg | Alzheimer's brain. ([[WC]]/NIH)
Image:AD versus CO.jpg | Alzheimer's brain macroscopy (top) vs control (bottom). (WC/Hersenbank)
File:Alois Alzheimer 002.jpg | Alois Alzheimer provided a first description of the pathology. (NLM)
</gallery>
 
===Microscopic===
Features:
#Neurofibrillary tangles.
#*Consists of ''tau''.
#*Location: hippocampus, cerebral cortex, hypothalamus.
#*Dementia severity correlates better with NF tangles number than senile plaque number.<ref>{{Ref PBoD8|1317}}</ref>
#*Six-tiered scoring method to assess tangle load <ref>{{Cite journal  | last1 = Braak | first1 = H. | last2 = Braak | first2 = E. | title = Neuropathological stageing of Alzheimer-related changes. | journal = Acta Neuropathol | volume = 82 | issue = 4 | pages = 239-59 | month =  | year = 1991 | doi =  | PMID = 1759558 }}</ref>
#*Images: [http://www.pakmed.net/academic/age/alz/plaques_tanglesBorder.jpg tangles - schematic (pakmed.net)]<ref name=pakmednet>URL: [http://www.pakmed.net/academic/age/alz/alz030.htm http://www.pakmed.net/academic/age/alz/alz030.htm]. Accessed on: 12 November 2010.</ref>, [http://faculty.washington.edu/alexbert/MEDEX/Fall/adtangle.jpg tangle (washington.edu)].<ref name=alexbert>URL: [http://faculty.washington.edu/alexbert/MEDEX/Fall/NeuroPath_Obj.htm http://faculty.washington.edu/alexbert/MEDEX/Fall/NeuroPath_Obj.htm]. Accessed on: 13 November 2010.</ref>
#Senile plaques ([[AKA]] neuritic plaques).
#*Consists of two components:
#*#Centre - radiates.
#*#*Consists of Abeta amyloid
#*#Neurites - swollen axons.
#*Considered to be more specific for Alzheimer's than NF tangles.
#**How to remember: '''s'''enile '''p'''laques = '''sp'''ecific.
#*There is a CERAD staging system for senile plaque load: 0 (none), I (mild), II (moderate), III (severe).<ref>{{Cite journal  | last1 = Mirra | first1 = SS. | last2 = Heyman | first2 = A. | last3 = McKeel | first3 = D. | last4 = Sumi | first4 = SM. | last5 = Crain | first5 = BJ. | last6 = Brownlee | first6 = LM. | last7 = Vogel | first7 = FS. | last8 = Hughes | first8 = JP. | last9 = van Belle | first9 = G. | title = The Consortium to Establish a Registry for Alzheimer's Disease (CERAD). Part II. Standardization of the neuropathologic assessment of Alzheimer's disease. | journal = Neurology | volume = 41 | issue = 4 | pages = 479-86 | month = Apr | year = 1991 | doi =  | PMID = 2011243 }}</ref>
#*Images: [http://library.med.utah.edu/WebPath/jpeg5/CNS091.jpg senile plaques (utah.edu)]<ref>URL: [http://library.med.utah.edu/WebPath/EXAM/IMGQUIZ/npfrm.html http://library.med.utah.edu/WebPath/EXAM/IMGQUIZ/npfrm.html]. Accessed on: 5 December 2010.</ref> [http://commons.wikimedia.org/wiki/File:Cerebral_amyloid_angiopathy_-2a-_amyloid_beta_-_high_mag.jpg senile plaques - beta-APP - high mag. (WC)].
#Neuron loss.
#+/-[[Cerebral amyloid angiopathy]].
 
====Images====
<gallery>
Image:Neuritic plaque HE stain.jpg | Neuritic plaques with amyloid core in HE. (WC/jensflorian)
Image:Alzheimer neuritic plaque gallyas stain.jpg | Neuritic plaques in Gallays silver impregnation. (WC/jensflorian)
Image:Alzheimer dementia (3) presenile onset.jpg | Neuritic plaques with amyloid core in Bodian stain. (WC/KGH)
Image:Cerebral amyloid angiopathy -2a- amyloid beta - high mag.jpg | Plaques with Abeta IHC. (WC/Nephron)
Image:Neurofibrillary tangles in the Hippocampus of an old person with Alzheimer-related pathology, HE 3.JPG | Neurofibrillary tangles in HE. (WC/Patho)
File:Neurofibrillary tangles in the Hippocampus of an old person with Alzheimer-related pathology, immunohistochemistry for tau protein.JPG | Tau IHC highlighting tangles. (WC/Patho)
File:Neurofibrillary tangles in the Hippocampus of an old person with Alzheimer-related pathology, Gallyas silver stain.JPG | Tangles in Gallays silver impregnation.(WC/Patho)
File:Hirano bodies in the Hippocampus in an old person with Alzheimer-related pathology, HE 2.JPG | HE stain with ghost tangles and Hirano bodies in AD. (WC/Patho)
File:Granulovacuolar degeneration.JPG | HE stain with granulovaculolar degeneration in AD. (WC/Patho)
</gallery>
 
===Classification===
NIA/AA Guidelines: "ABC" scoring method <ref>{{Cite journal  | last1 = Montine | first1 = TJ. | last2 = Phelps | first2 = CH. | last3 = Beach | first3 = TG. | last4 = Bigio | first4 = EH. | last5 = Cairns | first5 = NJ. | last6 = Dickson | first6 = DW. | last7 = Duyckaerts | first7 = C. | last8 = Frosch | first8 = MP. | last9 = Masliah | first9 = E. | title = National Institute on Aging-Alzheimer's Association guidelines for the neuropathologic assessment of Alzheimer's disease: a practical approach. | journal = Acta Neuropathol | volume = 123 | issue = 1 | pages = 1-11 | month = Jan | year = 2012 | doi = 10.1007/s00401-011-0910-3 | PMID = 22101365 }}</ref>
* (A) assessment of amyloid b deposits
* (B) staging of neurofibrillary tangles
* (C) scoring of neuritic plaques
 
{| class="wikitable"
|-
! (A) abeta plaques (Thal phase)<ref>{{Cite journal  | last1 = Thal | first1 = DR. | last2 = Rüb | first2 = U. | last3 = Orantes | first3 = M. | last4 = Braak | first4 = H. | title = Phases of A beta-deposition in the human brain and its relevance for the development of AD. | journal = Neurology | volume = 58 | issue = 12 | pages = 1791-800 | month = Jun | year = 2002 | doi =  | PMID = 12084879 }}</ref>
! (B) Neurofibrillary tangles (Braak stage) <ref>{{Cite journal  | last1 = Braak | first1 = H. | last2 = Braak | first2 = E. | title = Neuropathological stageing of Alzheimer-related changes. | journal = Acta Neuropathol | volume = 82 | issue = 4 | pages = 239-59 | month =  | year = 1991 | doi =  | PMID = 1759558 }}</ref>
! (C) neuritic plaques (CERAD) <ref>{{Cite journal  | last1 = Mirra | first1 = SS. | last2 = Heyman | first2 = A. | last3 = McKeel | first3 = D. | last4 = Sumi | first4 = SM. | last5 = Crain | first5 = BJ. | last6 = Brownlee | first6 = LM. | last7 = Vogel | first7 = FS. | last8 = Hughes | first8 = JP. | last9 = van Belle | first9 = G. | title = The Consortium to Establish a Registry for Alzheimer's Disease (CERAD). Part II. Standardization of the neuropathologic assessment of Alzheimer's disease. | journal = Neurology | volume = 41 | issue = 4 | pages = 479-86 | month = Apr | year = 1991 | doi =  | PMID = 2011243 }}</ref>
|-
| (A0) 0
| (B0) 0
| (C0) none
|-
| (A1) 1 (temporal),2 (+frontal, +CA1)
| (B1) I,II (transentorhinal)
| (C1) sparse (1–5 neuritic plaques/1 mm2)
|-
| (A2) 3 (+diencephalon, +striatum)
| (B2) III,IV (limbic)
| (C2) moderate(6–19 neuritic plaques/1 mm2)
|-
| (A3) 4 (+brainstem),5 (+cerebellum, +pons)
| (B3) V,VI (neocortical)
| (C3) frequent(>20 neuritic plaques/1 mm2)
|}
The ABC score is a good indicator for the likelihood of dementia.
 
Example:
Cerebellar abeta deposits (A3) +  tangles in entorhinal cortex and few temporal (B2), + 15 neuritic plaques per 1 mm2 (C2) -> (A3, B3, C2): intermediate  AD level change.
 
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.
 
==Prion diseases==
===General===
Etiology:<ref name=pmid16609731>{{cite journal |author=Watts JC, Balachandran A, Westaway D |title=The expanding universe of prion diseases |journal=PLoS Pathog. |volume=2 |issue=3 |pages=e26 |year=2006 |month=March |pmid=16609731 |pmc=1434791 |doi=10.1371/journal.ppat.0020026 |url=}}</ref>
*Misfolded cell-surface protein called PrP<sup>SC</sup>.
**This is derived from the protein ''PrP<sup>C</sup>'' encoded by the ''PRNP'' gene.
*Different genetics strains are associated with varying clinical phenotype.<ref>{{Cite journal  | last1 = Monari | first1 = L. | last2 = Chen | first2 = SG. | last3 = Brown | first3 = P. | last4 = Parchi | first4 = P. | last5 = Petersen | first5 = RB. | last6 = Mikol | first6 = J. | last7 = Gray | first7 = F. | last8 = Cortelli | first8 = P. | last9 = Montagna | first9 = P. | title = Fatal familial insomnia and familial Creutzfeldt-Jakob disease: different prion proteins determined by a DNA polymorphism. | journal = Proc Natl Acad Sci U S A | volume = 91 | issue = 7 | pages = 2839-42 | month = Mar | year = 1994 | doi = 10.1073/pnas.91.7.2839 | PMID = 7908444 }}</ref>
 
 
Includes:
*Creutzfeldt-Jakob disease (CJD).
*Sporadic fatal insomnia (sFI).<ref name=pmid16609731>{{cite journal |author=Watts JC, Balachandran A, Westaway D |title=The expanding universe of prion diseases |journal=PLoS Pathog. |volume=2 |issue=3 |pages=e26 |year=2006 |month=March |pmid=16609731 |pmc=1434791 |doi=10.1371/journal.ppat.0020026 |url=}}</ref>
*Fatal familial insomnia (FFI).<ref name=Ref_PCPBoD8_672>{{Ref PCPBoD8|672}}</ref><ref name=omim600072>{{OMIM|600072}}</ref>
*Gestmann-Straussler-Scheinker syndrome (GSS) - due to PRNP gene mutations.<ref name=Ref_PCPBoD8_671>{{Ref PCPBoD8|671}}</ref>
 
===IHC===
PrP<sup>C</sup>:<ref name=Ref_PCPBoD8_672>{{Ref PCPBoD8|672}}</ref>
*Congo red +ve.
*PAS +ve.
 
==Creutzfeldt-Jakob disease==
*Commonly abbreviated as ''CJD''.
===General===
*Rare.
*Incurable disease.
 
Usually diagnosed clinically:
*Characteristic findings:
**Very rapid decline (3-4 months).
**Characteristic (cortex findings on) neuroradiology.
 
====Variant Creutzfeldt-Jakob disease====
*Abbreviated ''vCJD''.
=====General=====
*Associated with ''bovine spongiform encephalopathy'' ([[AKA]] ''mad cow disease'').
*Should sample: [[spleen]], [[lymph node]]s, tonsils.<ref name=Ref_HospAuto83>{{Ref HospAuto|83}}</ref>
 
===Microscopic===
Features:
*Spongy appearance (cytoplasmic vacuolization<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/opaq/PathQuiz/N0I002-PQ01-M.htm http://moon.ouhsc.edu/kfung/jty1/opaq/PathQuiz/N0I002-PQ01-M.htm]. Accessed on: 19 October 2010.</ref>).
 
Note:
*Spongiform changes may be seen in [[ALS]], [[Alzheimer's disease]] and Lewy body disease (e.g. [[Parkinson disease]]); however, the changes are only in the upper cortex and not diffuse.<ref>{{Ref APBR|419 Q4}}</ref>
 
===Molecular===
*The CJD phenotype is associated with a PRNP D178N mutation and valine polymorphism at codon 129 (D178N-129V).
** Note: A Met129 polymorphism will cause Fatal familiar insomnia in the setting of the same PRNP D178N mutation. <ref>{{Cite journal  | last1 = Goldfarb | first1 = LG. | last2 = Petersen | first2 = RB. | last3 = Tabaton | first3 = M. | last4 = Brown | first4 = P. | last5 = LeBlanc | first5 = AC. | last6 = Montagna | first6 = P. | last7 = Cortelli | first7 = P. | last8 = Julien | first8 = J. | last9 = Vital | first9 = C. | title = Fatal familial insomnia and familial Creutzfeldt-Jakob disease: disease phenotype determined by a DNA polymorphism. | journal = Science | volume = 258 | issue = 5083 | pages = 806-8 | month = Oct | year = 1992 | doi = 10.1126/science.1439789 | PMID = 1439789 }}</ref>
 
 
<gallery>
Image:SpongiformChangeCJD.jpg | CJD. (WC/DRdoubleB)
File:Variant Creutzfeldt-Jakob disease (vCJD), H&E.jpg|Spongiform changes in CJD. (CDC/ Teresa Hammett)
File:Variant CJD HE.jpg | Florid plaques in vCJD. (WC/Sbrandner)
File:Cdc cjd2.jpg | Florid plaques in vCJD - low mag. (WC/CDC.gov)
Image:VCJD_Tonsil.jpg | vCJD - prion protein immunostain tonsil. (WC/Sbrandner)
File:CJD PRP cortex.jpg | sCJD - prion protein immunostain cortex. (WC/jensflorian)
File:CJD PRP cerebellum.jpg | sCJD - prion protein immunostain cerebellum. (WC/jensflorian)
</gallery>
*[http://path.upmc.edu/cases/case86.html CJD - several cases (upmc.edu)].


Etiology:
=Alpha-synucleinopathies=
*Alpha-synuclein.
Without clincial information [[Parkinson's disease]] and [[Dementia with Lewy bodies]] cannot separated in histology.


Clinical features of Dementia with Lewy bodies:  
==Dementia with Lewy bodies==
===General===
Clinical features:  
*Parkinsonian features.
*Parkinsonian features.
*Hallucinations (visual).
*Hallucinations (visual).
*Progressive cognitive decline with fluctuations.
*Progressive cognitive decline with fluctuations.
===Microscopic===
Features:
*[[Lewy bodies]].
*Lewy neurites.
Note: Cortical Lewy bodies are easily missed in HE.
===IHC===
*Alpha-synuclein +ve.
===Images===
<gallery>
File:DLB frontal lewy bodies HE.jpg | Lewy bodies in frontal cortex of DLB. (WC/jensflorian)
File:A synuclein cortex DLB.jpg | Alpha-synculein IHC showing cortical Lewy bodies. (WC/jensflorian)
File:Lewy neurites alpha synuclein.jpg | Alpha-synculein IHC showing Lewy Neurites in DLB. (WC/jensflorian)
</gallery>
==Parkinson disease==
===General===
*Common - often sporadic.
*May be genetic.
Clinical ''TRAP'':<ref>URL: [http://www.nysslha.org/i4a/pages/index.cfm?pageid=3519 http://www.nysslha.org/i4a/pages/index.cfm?pageid=3519]. Accessed on: 30 March 2011.</ref>
*Tremor.
*Rigidity.
*Akinesia.
*Postural instability.
Genetics:<ref name=Ref_PCPBoD8_677>{{Ref PCPBoD8|677}}</ref>
*LRRK2 gene<ref name=omim609007>{{OMIM|609007}}</ref> - autosomal dominant.
*PARK2 gene (parkin)<ref name=omim602544>{{OMIM|602544}}</ref> - autosomal recessive.
===Gross===
Features:<ref name=Ref_PBoD8_1319>{{Ref PBoD8|1319}}</ref>
*Abnormally pale substantia nigra.
**Pigmentation increases with age.
*Pale ''[[locus ceruleus]]''.
Notes:
*Substantia nigra is a midbrain structure.
**Image: [http://commons.wikimedia.org/wiki/File:Midbraincrosssection.png Midbrain - schematic (WC)].
===Microscopic===
Features:<ref name=Ref_PBoD8_1319>{{Ref PBoD8|1319}}</ref>
*Loss of pigmented (catecholaminergic) neurons in the substantia nigra and locus ceruleus.
*Gliosis - due to neuron loss.
*[[Lewy bodies]] (in remaining neurons) - '''key feature'''.
**Eosinophilic cytoplasmic inclusion with "dense" (darker) core and pale (surrounding) halo.
***Consist of filaments composed of alpha-synuclein.
*Lewy neurites - alpha-synuclein positive processes.
===IHC===
*Alpha-synuclein +ve.
===Images===
<gallery>
File:Journal.pone.0008247.g001.png | Schematic progression of PD (PLOSone/Jubault et al.).
File:Histological sample of Substantia nigra in Parkinson's disease.jpg | Lewy body (HE, left) and Lewy neurite (aSyn IHC, right).
File:Lewy Body alphaSynuclein.jpg | Alpha-synculein positive Lewy body (WC/Marvin101).
File:Lewy bodies (alpha synuclein inclusions).jpg | Lewy body and Lewy neurites (WC/Suraj Rajan).
</gallery>
===Molecular===
*Hereditary forms in less than 10% of the cases
**Involved genes are consecutively labeled PARK1, PARK2....


==Multiple system atrophy==
==Multiple system atrophy==
Multiple system atrophy is a neurodegenerative disease of the parkinsonism-plus disorder group.
===General===
Clinical findings variable:
Clinical findings variable:
*Parkinsonism (stiatonigral degeneration).
*Parkinsonism (stiatonigral degeneration, MSA-P).
*Ataxia (olivo-panto-cerebellar degeneration).
*Ataxia (olivo-ponto-cerebellar degeneration, MSA-C).
*Autonomic dysfunction (Shy-Drager syndrome, depreceated).
*Clinical onset between 40-60 years.
* Progedient tremor, atxia, laryngeal paresis, wakness, cognitive decline.
* Patients usually succumb after 6 years from aspiration pneumonia.
 
DDx:
* [[Spinocerebellar ataxia]].
* [[Parkinson disease]].
* Motor-neuron disease.
* [[Lewy-Body disease]].
 
===Macroscopy===
* Cerebral (mild) & cerebellar atrophy.
* greenish [[putamen]].
* Discoloration [[Substantia nigra]] and [[Locus coeruleus]]
 
===Microscopic===
Features:
*Inclusions cerebral, subcortical white matter, cerebellar.
*Neuronal loss and gliosis (absent in minimal-change MSA).
*Alpha-synuclein-rich glial and neuronal cytoplasmic inclusions in white matter (finding at autopsy).<ref name=pmid18825660>{{Cite journal  | last1 = Wenning | first1 = GK. | last2 = Stefanova | first2 = N. | last3 = Jellinger | first3 = KA. | last4 = Poewe | first4 = W. | last5 = Schlossmacher | first5 = MG. | title = Multiple system atrophy: a primary oligodendrogliopathy. | journal = Ann Neurol | volume = 64 | issue = 3 | pages = 239-46 | month = Sep | year = 2008 | doi = 10.1002/ana.21465 | PMID = 18825660 }}</ref>
**Inclusions in oligodendrocytes (triangular, flame-like or sickle-shaped) are definitive diagnostic for MSA.<ref>MUN. 16 November 2010.</ref><ref>{{cite journal |authors=Trojanowski JQ, Revesz T |title=Proposed neuropathological criteria for the post mortem diagnosis of multiple system atrophy |journal=Neuropathol. Appl. Neurobiol. |volume=33 |issue=6 |pages=615–20 |year=2007 |pmid=17990994 |doi=10.1111/j.1365-2990.2007.00907.x |url=}}</ref>
**Inclusions usu. abundant in basal ganglia, substantia nigra, pontine nuclei, medulla and cerebellum.
*Pons and Putamen:
** Nuclear inclusions (sparse in most cases).
** Neuropil threads (alpha-synuclein).
*Loss of myelinated fibers from external capsule, striatum and pallidum.
 
===Images===
<gallery>
File:Msa_macroscopy_putamen_discoloration.jpg | Gray-brown discoloration in putamen of a striatonigral-type MSA (WC/jensflorian).
File:MSA Gallays Papp Lantos inclusions.jpg | Gallays silver stain showing MSA-typic inclusions (WC/jensflorian).
File:MSA aSynuclein.jpg | a-synuclein IHC showing Glial and neuronal cytoplasmic inclusion in the pons of a MSA case (WC/jensflorian).
</gallery>
 
===Molecular===
* No known alpha-synuclein mutation.
* Genetic variants of SNCA gene assoicated with MSA. <ref name=PMID2743996>{{Cite journal  | last1 = Pimenta | first1 = PF. | last2 = da Silva | first2 = RP. | last3 = Sacks | first3 = DL. | last4 = da Silva | first4 = PP. | title = Cell surface nanoanatomy of Leishmania major as revealed by fracture-flip. A surface meshwork of 44 nm fusiform filaments identifies infective developmental stage promastigotes. | journal = Eur J Cell Biol | volume = 48 | issue = 2 | pages = 180-90 | month = Apr | year = 1989 | doi =  | PMID = 2743996 }}</ref>
 
=Tauopathies=
More than 20 different degenerative disorders can be classified as tauopathies.<ref>{{Cite journal  | last1 = Williams | first1 = DR. | title = Tauopathies: classification and clinical update on neurodegenerative diseases associated with microtubule-associated protein tau. | journal = Intern Med J | volume = 36 | issue = 10 | pages = 652-60 | month = Oct | year = 2006 | doi = 10.1111/j.1445-5994.2006.01153.x | PMID = 16958643 }}</ref> '''FTLD-tau''' is an umbrella term used for tauopathies including PSP, CBD, PiD and GGT. <ref>{{Cite journal  | last1 = Forrest | first1 = SL. | last2 = Kril | first2 = JJ. | last3 = Stevens | first3 = CH. | last4 = Kwok | first4 = JB. | last5 = Hallupp | first5 = M. | last6 = Kim | first6 = WS. | last7 = Huang | first7 = Y. | last8 = McGinley | first8 = CV. | last9 = Werka | first9 = H. | title = Retiring the term FTDP-17 as MAPT mutations are genetic forms of sporadic frontotemporal tauopathies. | journal = Brain | volume = 141 | issue = 2 | pages = 521-534 | month = Feb | year = 2018 | doi = 10.1093/brain/awx328 | PMID = 29253099 }}</ref>
 
 
==Argyrophilic grain disease==
 
==Corticobasal degeneration==
*AKA '''CBD'''.
*Symptoms may vary:
**Progressive asymmetrical rigidity and apraxia, progressive aphasia or dementia.
*Neuronal and glial Tau-positive inclusions.<ref>{{Cite journal  | last1 = Dickson | first1 = DW. | last2 = Bergeron | first2 = C. | last3 = Chin | first3 = SS. | last4 = Duyckaerts | first4 = C. | last5 = Horoupian | first5 = D. | last6 = Ikeda | first6 = K. | last7 = Jellinger | first7 = K. | last8 = Lantos | first8 = PL. | last9 = Lippa | first9 = CF. | title = Office of Rare Diseases neuropathologic criteria for corticobasal degeneration. | journal = J Neuropathol Exp Neurol | volume = 61 | issue = 11 | pages = 935-46 | month = Nov | year = 2002 | doi =  | PMID = 12430710 }}</ref>
**Astrocytic plaques.
**Thread-like lesions and coiled bodies.
**Ballooned neurons +/-.
*Pathology is cortical and striatal and Gallyas-positive.
*Neuronal loss in the substantia nigra.
 
DD: PSP (widespread  neurofibrillary degeneration, with characteristic globose NFT).
 
==Globular glial tauopathies==
*Commonly abbreviated ''GGT''.
*AKA ''sporadic multiple system tauopathy''.
*Rare disease.<ref>{{Cite journal  | last1 = Ahmed | first1 = Z. | last2 = Bigio | first2 = EH. | last3 = Budka | first3 = H. | last4 = Dickson | first4 = DW. | last5 = Ferrer | first5 = I. | last6 = Ghetti | first6 = B. | last7 = Giaccone | first7 = G. | last8 = Hatanpaa | first8 = KJ. | last9 = Holton | first9 = JL. | title = Globular glial tauopathies (GGT): consensus recommendations. | journal = Acta Neuropathol | volume = 126 | issue = 4 | pages = 537-544 | month = Oct | year = 2013 | doi = 10.1007/s00401-013-1171-0 | PMID = 23995422 }}</ref>
*Combination of frontotemporal dementia and motor neuron disease or only part thereof.
*4-repeat tauopathy.
 
===Microscopic===
*Globular oligodendroglial and astrocytic Tau inclusions.
*Absence of tufted astrocytes.
*Mostly Gallyas-negative.


Etiology:
*Alpha-synuclein-rich glial cytoplasmic inclusions - finding at autopsy.<ref name=pmid18825660>{{Cite journal  | last1 = Wenning | first1 = GK. | last2 = Stefanova | first2 = N. | last3 = Jellinger | first3 = KA. | last4 = Poewe | first4 = W. | last5 = Schlossmacher | first5 = MG. | title = Multiple system atrophy: a primary oligodendrogliopathy. | journal = Ann Neurol | volume = 64 | issue = 3 | pages = 239-46 | month = Sep | year = 2008 | doi = 10.1002/ana.21465 | PMID = 18825660 }}</ref>
**Inclusions in oligodendrocytes.<ref>MUN. 16 November 2010.</ref>


==Progressive supranuclear palsy==
==Progressive supranuclear palsy==
*Commonly abbreviated ''PSP''.
*[[AKA]] ''Steele-Richardson-Olszewski syndrome''.
===General===
===General===
*[[AKA]] ''Steele-Richardson-Olszewski syndrome''.
*Diagnosis - clinical.<ref name=psp_emedicine>URL: [http://emedicine.medscape.com/article/1151430-overview http://emedicine.medscape.com/article/1151430-overview]. Accessed on: 11 November 2010.</ref>
*Diagnosis: clinical.<ref name=psp_emedicine>URL: [http://emedicine.medscape.com/article/1151430-overview http://emedicine.medscape.com/article/1151430-overview]. Accessed on: 11 November 2010.</ref>
 
Clinical:
*Impaired control of gaze, esp. difficulty looking up and down (supranuclear palsy).<ref name=pmid21690028>{{Cite journal  | last1 = Levy | first1 = R. | title = [Progressive supranuclear palsy: what's new?]. | journal = Geriatr Psychol Neuropsychiatr Vieil | volume = 9 | issue = 2 | pages = 191-201 | month = Jun | year = 2011 | doi = 10.1684/pnv.2011.0271 | PMID = 21690028 }}</ref>
*Parkinsonism.<ref name=pmid22228724>{{Cite journal  | last1 = Bertram | first1 = K. | last2 = Williams | first2 = DR. | title = Visual hallucinations in the differential diagnosis of parkinsonism. | journal = J Neurol Neurosurg Psychiatry | volume = 83 | issue = 4 | pages = 448-52 | month = Apr | year = 2012 | doi = 10.1136/jnnp-2011-300980 | PMID = 22228724 }}</ref>


===Microscopic===
===Microscopic===
Line 184: Line 598:
*Globose neurofibrillary tangles in neurons.
*Globose neurofibrillary tangles in neurons.
*Coiled bodies in oligodendrocytes.
*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.<ref>URL: [http://neuropathologyblog.blogspot.com/2008/03/grumose-degeneration-in-cerebellar.html http://neuropathologyblog.blogspot.com/2008/03/grumose-degeneration-in-cerebellar.html]. Accessed on: 4 December 2010.</ref><ref>{{cite journal |author=Yamanouchi H, Yokoo H, Yuhara Y, ''et al.'' |title=An autopsy case of ornithine transcarbamylase deficiency |journal=Brain Dev. |volume=24 |issue=2 |pages=91–4 |year=2002 |month=March |pmid=11891099 |doi= |url=}}</ref>
Images:
*[http://path.upmc.edu/cases/case238/micro.html PSP - several images (upmc.edu)].
==Pick disease==
===General===
*Dementia.
===Gross===
*Frontal and temporal lobe atrophy.<ref name=Ref_PCPBoD8_676>{{Ref PCPBoD8|676}}</ref>
**May be called "walnut brain"<ref>URL: [http://medical-dictionary.thefreedictionary.com/Walnut+Brain http://medical-dictionary.thefreedictionary.com/Walnut+Brain]. Accessed on: 14 March 2012.</ref> - as it resembles a walnut.
===Microscopic===
Features:<ref name=Ref_PCPBoD8_676>{{Ref PCPBoD8|676}}</ref>
*Pick cells = large ballooned neurons.
*Pick bodies = round, homogenous, intracytoplasmic inclusions, size ~10 micrometers.
Image(s):
*[http://www.nature.com/nrneurol/journal/v6/n2/fig_tab/nrneurol.2009.216_F1.html Pick body (nature.com)].<ref name=pmid20139998>{{Cite journal  | last1 = Grossman | first1 = M. | title = Primary progressive aphasia: clinicopathological correlations. | journal = Nat Rev Neurol | volume = 6 | issue = 2 | pages = 88-97 | month = Feb | year = 2010 | doi = 10.1038/nrneurol.2009.216 | PMID = 20139998 }}</ref>
=TDP Proteinopathies=
==FTLD-TDP==
*Accounts for about 50% of all FTLD cases.
*Degeneration of frontal and temporal lobes.
*Inclusions not seen in HE or silver stains.
*TDP43-positive
**Neuronal cytoplasmic inclusions.
**Neuronal intranuclear inclusions.
**Dystrophic neurites.
*Ubiquitin+ve.
*p62+ve.
*aSynculein-ve.
*Tau-ve.
*FUS-ve.
*Four FTLD-TDP subtypes
** Type A: compact nuclear/cytoplasmatic inclusions, associated with GRN mutations.
** Type B: diffuse nuclear/cytoplasmatic inclusions most often seen in C9orf72 expansion.
** Type C: dystrophic neurites.
** Type D: Lentiform nuclear inclusions, only in cases with VCP mutations.
*C9orf72 mutated show additional DPR+ve staining of TDP‐43‐ve inclusions.
**These addtional inclusions are ubiquitin+ve and p62+ve
=FTLD-FET=
* Clinical manifestations depend on the distribution of the pathologic alterations in the CNS
* Currently 3 disorders among the FTLD-FET subgroup.
* In contrast to ALS-FUS, no genetic alterations of FUS have been reported to date for cases within the FTLD-FUS group.
* 5–10% of all FTLD cases
* Deposited Proteins: FUS, EWS, TAF-15.
* FUS‐positive inclusions in FTLD cases show co‐aggregation of TAF15 and EWS
**(Different from ALS-FUS)
DDx (also FUS+ve):
*Spinocerebellar Ataxia (SCA)
*Huntington Disease (SD)
==Atypical FTLD‐U==
* Early onset frontotemporal dementia, rapidly progressive psycho‐behavioural changes.
* Neuronal cytoplasmic inclusions in hippocampus and frontotemporal lobes.
* Ubiquitin+ve, tau/TDP‐ve.
* FET+ve inclusions
** Unique vermiform filamentous neuronal nuclear inclusions.
* Caudate nucleus head degeneration and hippocampal sclerosis.
==Basophilic inclusion body disease==
* AKA: BIBD.
* Variable clinic (behavioral, cognitive alterations, parkinsonism, motor neuron diseases, ALS-like).
* Age of onset: 35-70 years.
* Intraneuronal cytoplasmic basophilic inclusion bodies.
* FUS+ve (universally).
* EWS+ve.
* TAF15+ve.
* alpha-Internexin+ve.
==Neuronal Intermediate Filament Inclusion Disease==
* AKA: NIFID.
* Sporadic early‐onset frontotemporal dementia, motor neuron disease, extrapyramidal motor symptoms.
* Hyaline conglomerates (brightly eosinophilic branching fibrillar structures embedded in a round, well-delineated, glassy vacuole).
* Deposits in cerebral cortex, hippocampus, basal ganglia, thalamus, cerebellar dentate, numerous brainstem nuclei and lower motor neurons.
* FUS+ve/EWS+ve/TAF15+ve (heterogenous).
** FET+ve filamentous nuclear inclusions in the hippocampus.
* Ubiquitin +/-ve.
* NF +ve (some subunits).
* p62 +/-ve.
* TDP43-ve.
* Tau-ve.
* α-synuclein-ve.
=Other=
==Chronic traumatic encephalopathy==
*Abbreviated ''CTE''.
{{Main|Chronic traumatic encephalopathy}}


==Huntington disease==
==Huntington disease==
===General===
===General===
*Autosomal dominant inheritance.
*Autosomal dominant inheritance.
*Mutation: unstable CAG repeat.<ref name=pmid20360611>{{cite journal |author=Kumar P, Kalonia H, Kumar A |title=Huntington's disease: pathogenesis to animal models |journal=Pharmacol Rep |volume=62 |issue=1 |pages=1–14 |year=2010 |pmid=20360611 |doi= |url=}}</ref>
*Mutation in ''Huntington gene'' (HTT):<ref name=pmid20360611>{{cite journal |author=Kumar P, Kalonia H, Kumar A |title=Huntington's disease: pathogenesis to animal models |journal=Pharmacol Rep |volume=62 |issue=1 |pages=1–14 |year=2010 |pmid=20360611 |doi= |url=}}</ref>
**11-34 CAG repeat = normal.<ref name=omim613004>{{OMIM|613004}}</ref>
**>42 CAG repeat = Huntington disease.
 
Clinical:<ref name=Ref_APBR415>{{Ref APBR|415 Q44}}</ref>
*Early onset dementia.
*Involuntary movements (chorea) - both arms and legs.
*Behaviour changes, e.g. grimacing.
*Speech changes.
 
===Gross===
===Gross===
*Missing caudate.<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm]. Accessed on: 29 October 2010.</ref>
*Severe caudate atrophy.<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm]. Accessed on: 29 October 2010.</ref>
**Prominent frontal horns of the lateral ventricles.<ref>URL: [http://path.upmc.edu/cases/case117/gross.html http://path.upmc.edu/cases/case117/gross.html]. Accessed on: 3 January 2012.</ref>


Image: [http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm Huntington's disease (ouhsc.edu)].
Note:
*A normal caudate bulges into the ventricle.


==Binswanger's disease==
Images:
*[http://moon.ouhsc.edu/kfung/jty1/NeuroTest/Q07-Ans.htm Huntington's disease (ouhsc.edu)].
*[http://path.upmc.edu/cases/case117/gross.html Prominent frontal horns of the lateral ventricles (upmc.edu)].
 
===Microscopic===
Features:<ref name=Ref_APBR415>{{Ref APBR|415 Q44}}</ref>
*Neuron loss.
*Gliosis.
 
==Binswanger disease==
===General===
===General===
*Multi-infarct dementia affecting subcortical white matter.
*Multi-infarct dementia affecting subcortical white matter.
*Waste-basket diagnosis; diagnosed if [[CADASIL]] and amyloidosis have been excluded.
*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''.
*Diagnosis has been controversial -- most with this entity (in the past) were diagnosed with ''[[Alzheimer's disease]]''.


===Microscopic===
===Microscopic===
Line 204: Line 737:
*Subcortical lesions that replace the myelin consisting of macrophages.
*Subcortical lesions that replace the myelin consisting of macrophages.


==Prion diseases==
==Frontotemporal lobar degeneration with ubiquitinated inclusions==  
Etiology:<ref name=pmid16609731>{{cite journal |author=Watts JC, Balachandran A, Westaway D |title=The expanding universe of prion diseases |journal=PLoS Pathog. |volume=2 |issue=3 |pages=e26 |year=2006 |month=March |pmid=16609731 |pmc=1434791 |doi=10.1371/journal.ppat.0020026 |url=}}</ref>
Abbreviated ''FTLD with ubiquitinated inclusions'' or ''FTLD-TDP43''.
*Misfolded cell-surface protein called PrP(C).
===General===
*There are several forms of ''frontotemporal dementia''.
*Related to [[amyotrophic lateral sclerosis]] (ALS); also a TDP-43 pathology.<ref>{{OMIM|105400}}</ref>
**There are several subtypes of FTLD with TDP-43.
 
===Gross===
*Frontal and temporal lobe atrophy.
 
Image:
*[http://commons.wikimedia.org/wiki/File:Frontotemporal_degeneration.png FTLD (WC)].


Includes:<ref name=pmid16609731>{{cite journal |author=Watts JC, Balachandran A, Westaway D |title=The expanding universe of prion diseases |journal=PLoS Pathog. |volume=2 |issue=3 |pages=e26 |year=2006 |month=March |pmid=16609731 |pmc=1434791 |doi=10.1371/journal.ppat.0020026 |url=}}</ref>
==Amyotrophic lateral sclerosis==
*Creutzfeldt-Jakob disease (CJD).
*Abbreviated ''ALS''.
*Sporadic fatal insomnia (sFI).


==Creutzfeldt-Jakob disease==
===General===
===General===
*Commonly abbreviated as ''CJD''.
*[[AKA]] Lou Gehrig's disease.
*Rare.
*Characterized by motor neuron death.
*Incurable disease.
*May be familial and associated with ''C9orf72 expansion'', or ''SOD1'', ''FUS'' and ''TARDBP'' mutations.<ref name=Ref_PCPBoD8_679>{{Ref PCPBoD8|679}}</ref><ref>{{Cite journal  | last1 = Guerrero | first1 = EN. | last2 = Wang | first2 = H. | last3 = Mitra | first3 = J. | last4 = Hegde | first4 = PM. | last5 = Stowell | first5 = SE. | last6 = Liachko | first6 = NF. | last7 = Kraemer | first7 = BC. | last8 = Garruto | first8 = RM. | last9 = Rao | first9 = KS. | title = TDP-43/FUS in motor neuron disease: Complexity and challenges. | journal = Prog Neurobiol | volume = 145-146 | issue =  | pages = 78-97 | month =  | year =  | doi = 10.1016/j.pneurobio.2016.09.004 | PMID = 27693252 }}</ref>
*Pathological protein aggregates cause dysfunction of RNA-binding proteins.
 
===Clinical===
*Peak incidence: 50-60yrs.
*2-5 per 100,000 individuals worldwide.
*Dead after disease onset: Usu. 2-5yrs.
*Weakness (Progressive bulbar, limb, thoracic, and abdominal muscle atrophy).
*About 20% of ALS cases develop frontotemporal lobar degeneration (FTLD).
*Environmental toxins are discussed (Guam ALS).<ref>{{Cite journal  | last1 = Chernoff | first1 = N. | last2 = Hill | first2 = DJ. | last3 = Diggs | first3 = DL. | last4 = Faison | first4 = BD. | last5 = Francis | first5 = BM. | last6 = Lang | first6 = JR. | last7 = Larue | first7 = MM. | last8 = Le | first8 = TT. | last9 = Loftin | first9 = KA. | title = A critical review of the postulated role of the non-essential amino acid, β-N-methylamino-L-alanine, in neurodegenerative disease in humans. | journal = J Toxicol Environ Health B Crit Rev | volume = 20 | issue = 4 | pages = 1-47 | month =  | year = 2017 | doi = 10.1080/10937404.2017.1297592 | PMID = 28598725 }}</ref>
 
===Microscopic===
Features:<ref name=Ref_PCPBoD8_679>{{Ref PCPBoD8|679}}</ref><ref>{{Cite journal  | last1 = Saberi | first1 = S. | last2 = Stauffer | first2 = JE. | last3 = Schulte | first3 = DJ. | last4 = Ravits | first4 = J. | title = Neuropathology of Amyotrophic Lateral Sclerosis and Its Variants. | journal = Neurol Clin | volume = 33 | issue = 4 | pages = 855-76 | month = Nov | year = 2015 | doi = 10.1016/j.ncl.2015.07.012 | PMID = 26515626 }}</ref>
*Loss of the giant cells of Betz.
*Motor neurons with eosinophilic inclusions (''Bunina bodies'').
**PAS positive cytoplasmic inclusions.
*Motor neuron loss + reactive gliosis + neurogenic muscular atrophy.
**Loss of myelinated axons in the lateral and anterior columns of the spinal cord.
*Ubiquitinated cytoplasmic inclusions.<ref>{{Cite journal  | last1 = Leigh | first1 = PN. | last2 = Anderton | first2 = BH. | last3 = Dodson | first3 = A. | last4 = Gallo | first4 = JM. | last5 = Swash | first5 = M. | last6 = Power | first6 = DM. | title = Ubiquitin deposits in anterior horn cells in motor neurone disease. | journal = Neurosci Lett | volume = 93 | issue = 2-3 | pages = 197-203 | month = Nov | year = 1988 | doi =  | PMID = 2853844 }}</ref>
*[[TDP-43]] proteinopathy in motor neurons (90% of all sporadic ALS cases).
**SOD1-mutant cases are [[TDP-43]]-ve.<ref>{{Cite journal  | last1 = Nakamura | first1 = S. | last2 = Wate | first2 = R. | last3 = Kaneko | first3 = S. | last4 = Ito | first4 = H. | last5 = Oki | first5 = M. | last6 = Tsuge | first6 = A. | last7 = Nagashima | first7 = M. | last8 = Asayama | first8 = S. | last9 = Fujita | first9 = K. | title = An autopsy case of sporadic amyotrophic lateral sclerosis associated with the I113T SOD1 mutation. | journal = Neuropathology | volume = 34 | issue = 1 | pages = 58-63 | month = Feb | year = 2014 | doi = 10.1111/neup.12049 | PMID = 23773010 }}</ref>
*C9orf72 expansion cases: p62+ve, [[TDP-43]]-ve inclusions in the dentate gyrus, neocortex, and cerebellum.<ref>{{Cite journal  | last1 = Al-Sarraj | first1 = S. | last2 = King | first2 = A. | last3 = Troakes | first3 = C. | last4 = Smith | first4 = B. | last5 = Maekawa | first5 = S. | last6 = Bodi | first6 = I. | last7 = Rogelj | first7 = B. | last8 = Al-Chalabi | first8 = A. | last9 = Hortobágyi | first9 = T. | title = p62 positive, TDP-43 negative, neuronal cytoplasmic and intranuclear inclusions in the cerebellum and hippocampus define the pathology of C9orf72-linked FTLD and MND/ALS. | journal = Acta Neuropathol | volume = 122 | issue = 6 | pages = 691-702 | month = Dec | year = 2011 | doi = 10.1007/s00401-011-0911-2 | PMID = 22101323 }}</ref>
**FUS-mutant cases show FUS+ve, p62+ve (few) and [[TDP-43]]-ve inclusions.<ref>{{Cite journal  | last1 = Vance | first1 = C. | last2 = Rogelj | first2 = B. | last3 = Hortobágyi | first3 = T. | last4 = De Vos | first4 = KJ. | last5 = Nishimura | first5 = AL. | last6 = Sreedharan | first6 = J. | last7 = Hu | first7 = X. | last8 = Smith | first8 = B. | last9 = Ruddy | first9 = D. | title = Mutations in FUS, an RNA processing protein, cause familial amyotrophic lateral sclerosis type 6. | journal = Science | volume = 323 | issue = 5918 | pages = 1208-1211 | month = Feb | year = 2009 | doi = 10.1126/science.1165942 | PMID = 19251628 }}</ref>
 
Images:
*[http://jsp.umin.ac.jp/corepictures2007/18/o02/index.html Bunina body (umin.ac.jp)].
*[http://pathology.mc.duke.edu/neuropath/CNSlecture4/alsbunina.jpg Bunina body (duke.edu)].<ref>URL: [http://pathology.mc.duke.edu/neuropath/CNSlecture4/CNSlecture4.htm http://pathology.mc.duke.edu/neuropath/CNSlecture4/CNSlecture4.htm]. Accessed on: 30 August 2011.</ref>
*[http://path.upmc.edu/cases/case291.html ALS - several images (upmc.edu)].
 
<gallery>
File:ALS-TDP-HE.jpg | Motor neuron loss in ALS-TDP. (WC)
File:ALS-TDP-43_IHC.jpg | pTDP-43 positive inclusions in neurons. (WC)
</gallery>


*Usually diagnosed clinically.
DDx:
**Characteristic findings:
*Spinal muscular atrophy.
***Very rapid decline (3-4 months).
*Primary Lateral Sclerosis.
***Characteristic (cortex findings on) neuroradiology.  
*Hereditary Spastic Paraparesis (HSP).


====Variant Creutzfeldt-Jakob disease (vCJD)====
==Hallervorden-Spatz disease==
*Associated with bovine spongiform encephalopathy.
*[[AKA]] ''pantothenate kinase-associated neurodegeneration''.
*Should sample: spleen, lymph nodes, tonsils.<ref name=Ref_HospAuto83>{{Ref HospAuto|83}}</ref>
 
===General===
*Uncommon.


===Microscopic===
===Microscopic===
Features:
Features:<ref>URL: [http://path.upmc.edu/cases/case207/dx.html http://path.upmc.edu/cases/case207/dx.html]. Accessed on: 11 January 2012.</ref>
*Spongy appearance (cytoplasmic vacuolization<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/opaq/PathQuiz/N0I002-PQ01-M.htm http://moon.ouhsc.edu/kfung/jty1/opaq/PathQuiz/N0I002-PQ01-M.htm]. Accessed on: 19 October 2010.</ref>).
*Axonal spheroids.
*Iron deposition.
 
Images:
*[http://path.upmc.edu/cases/case207.html HSD - several images (upmc.edu)].


Images:
===Stains===
*[http://commons.wikimedia.org/wiki/File:SpongiformChangeCJD.jpg CJD (WC)].
*Prussian blue +ve.
*[http://commons.wikimedia.org/wiki/File:VCJD_Tonsil.jpg vCJD - IHC (WC)].


==See also==
=See also=
*[[Neuropathology]].
*[[Neuropathology]].
*[[Neurohistology]].
*[[Neurohistology]].


==References==
=References=
{{Reflist|2}}
{{Reflist|2}}


[[Category:Neuropathology]]
[[Category:Neuropathology]]

Latest revision as of 20:32, 24 May 2020

Neurodegenerative diseases is a big part of neuropathology. It includes some discussion of dementia.

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
 
FUS/EWS/TAF15

Common diseases

Amyloidoses:

  • Alzheimer disease (Abeta).

'Pure' tauopathies:

Synucleinopathies:[2]

TDP-43 proteinopathies:

FET proteinopathies:

  • Basophilic inclusion body disease (BIBD).
  • Neuronal intermediate filament inclusion disease (NIFID).
  • Atypical frontotemporal lobar degeneration with ubiquitin-positive inclusions (atypical FTLD-U).

Prionopathies:

  • Creutzfeldt-Jakob disease (PrP).

Note: Some people consider α-synuclein as a prion-like protein.[3]


Table

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

Disease Deposited protein Distribution Clinical Histology Image
Alzheimer disease Abeta (mutated APP) corticolimbic, usu.
spares occipital
dementia plaques, neurofibrillary tangles [1]
Creutzfeldt-Jakob disease PrPres (mutated PrP) cortical & basal ganglia dementia (rapid progression),
movement disorder
cytoplasmic vacuolization, PrP+ve plaques, Kuru plaques (MV2 variant) [2]
Parkinson disease alpha-synuclein brainstem parkinsonism Lewy bodies in substantia nigra and locus coeruleus [3] [4]
Dementia with
Lewy bodies
alpha-synuclein corticolimbic, brainstem dementia + parkinsonism Lewy bodies brainstem and cortical, tangles [5] [6]
Multiple system atrophy alpha-synuclein basal ganglia, brainstem, cerebellum parkinsonism, ataxia Papp-Lantos inclusions (cytoplasmic deposits in oligodendrocytes)[4] [7]
Amyotrophic lateral
sclerosis (ALS)
TDP-43 motor neurons spasticity, weakness motor neuron loss, TDP-43+ve, TAF15-ve, EWS-ve inclusions in motor neurons [8]
Frontotemporal lobar
degeneration with TDP-43 (FTLD-TDP)
TDP-43 cortex, basal ganglia dementia, focal cortical syndromes histology depends on (type 1-4), ubiquitin and TDP-43+ve, tau and FUS-ve [9]
Frontotemporal lobar
degeneration with FET (FTLD-FET)
FUS/EWS/TAF15 cortex, medulla, hippocampus, and motor cells of the spinal cord dementia, cases classified as aFTLD-U, NIFID and BIBD FUS+ve, TAF15+ve, EWS+ve cytoplasmic & intranuclear inclusions, neuritic threads [10]
Progressive supranuclear palsy (FTLD-tau) tau 4R basal ganglia, brainstem atypical parkinsonism with early gait instability, falls, and supranuclear gaze palsy tau-positive globose neurofibrillary tangles
in neurons, tufted astrocytes, coiled bodies
in oligodendrocytes
[11]
Pick disease (FTLD-tau) tau 3R corticolimbic dementia + focal
cortical syndrome
Intraneuronal argyrophilic inclusions (Pick body) [12]
Corticobasal degeneration (CBD) (FTLD-tau) tau 4R cortical, basal ganglia dementia + movement disorder (Parkinson-plus syndrome) ballooned neurons, astrocytic plaques, pretangles in basal nucleus [13]
Argryophilic grain disease (AGD) (FTLD-tau) tau 4R medial temporal lobe, limbic structures late-onset amnestic syndrome Argyrophilic grains (also found unspecific in elederly) [14]

Immunohistochemistry

Alpha-synuclein

Look for:

  • Lewy bodies (seen in Parkinson's Disease (PD), Dementia with Lewy bodies (DLB)) = round cytoplasmic eosinophilic body +/- pale halo.
  • Lewy neurites(seen in PD and DLB) = abnormal neurites with filaments similar to those found in Lewy bodies.
  • Glial cytoplasmatic inclusions (Papp-Lantos bodies) seen in mutisystem atrophy (MSA).
  • Beta amyloid in vessels seen in cerebral amyloid angiopathy (CAA).

Tau

  • AT8 = stains phosphorylated tau.[5]
    • AT = anti-tau.
    • Stains tau 4R and tau 3R.[6]

TDP-43

  • May accumulate due to a progranulin mutation.

Microscopic

Ubiquitin

  • Marks proteins for recycling.
  • Stains Barr bodies in hippocampal granule cells[9]


p62

  • p62; poli-ubiquitin-binding protein p62.[5]

Microscopic

Look for:

  • Lewy bodies and extracellular pigment in neuromelanin-containing nuclei (SN, LC, DVN) -> PD.
  • Spongiform vacuolation in the neuropil (seen in Prion disease and FTLD-TDP).
  • Neurofibrillar tangles (pyramidal layer of dentate gyrus).
  • Granulovacuolar degeneration (granules within cytoplasmic vacuoles, mainly in the hippocampal pyramidal neurons, seen in AD).
  • Cores of amyloid plaqyes.
  • Cotton wool plaques (seen in familiar AD).
  • Pick cells (balloned neurons in frontal cortex).
  • Pick bodies (granular layer of dentate gyrus).
  • Extensive astrogliosis (striatonigral degeneration, hepatic encephalopathy).
  • Corpora amylacea in the cornu ammonis may be increased in neurodegenerative diseases. [10]

Clinical perspective

  • Correlations between clinical signs and molecular can be poor.
    • Example: The MAPT A152T gene mutation may cause clinical symptoms matching AD, CBD, PSP and LBD.[11]

Dementia 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

Dementia mnemonic VITAMIN D VEST:[12]

  • 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).

Parkinsonism causes

Amyloidoses

Alzheimer disease

General

  • Onset: episodic memory loss.
  • Diagnosis is clinical & pathologic.
    • Pathologic finding alone are not diagnostic.
    • Onset, rate of progression and the development of pathology are highly variable.
  • Defined by:
    • Pathological accumulation of amyloid β (Aβ) into extracellular plaques.
    • Abnormally phosphorylated tau that accumulates intraneuronally forming neurofibrillary tangles (NFTs).
    • Clinicopathological correlation better for NFT than for Aβ.[21]
  • Seen in conjunction with vascular amyloid deposition; see cerebral amyloid angiopathy.
  • Evidence of possible iatrogenic transmission by cadaver-sourced growth hormone batches.[22][23]



Genetics

Genes associated with Alzheimer disease:[24]

  • Amyloid precursor protein (APP).
    • On chromosome 21 - may explain why Trisomy 21 (Down syndrome) increases the risk of Alzheimer disease.[25]
  • Presenilin 1 (PSEN1).[26]
  • Presenilin 2 (PSEN2).[27]
  • Apolipoprotein E (APOE)[28] - specifically the epsilon-4 allele.

Gross

Features:

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

Gross/microscopic - disease spread by NF tangles (staging):[29]

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

Minimal sampling:

  • Frontal, parietal & temporal lobe
  • Hippocampus and entorhinal cortex

Additional sampling:

  • Basal ganglia
  • Cerebellum
  • Midbrain (including substantia nigra)
  • Occipital cortex

Images

Microscopic

Features:

  1. Neurofibrillary tangles.
  2. Senile plaques (AKA neuritic 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.
      • How to remember: senile plaques = specific.
    • There is a CERAD staging system for senile plaque load: 0 (none), I (mild), II (moderate), III (severe).[34]
    • Images: senile plaques (utah.edu)[35] senile plaques - beta-APP - high mag. (WC).
  3. Neuron loss.
  4. +/-Cerebral amyloid angiopathy.

Images

Classification

NIA/AA Guidelines: "ABC" scoring method [36]

  • (A) assessment of amyloid b deposits
  • (B) staging of neurofibrillary tangles
  • (C) scoring of neuritic plaques
(A) abeta plaques (Thal phase)[37] (B) Neurofibrillary tangles (Braak stage) [38] (C) neuritic plaques (CERAD) [39]
(A0) 0 (B0) 0 (C0) none
(A1) 1 (temporal),2 (+frontal, +CA1) (B1) I,II (transentorhinal) (C1) sparse (1–5 neuritic plaques/1 mm2)
(A2) 3 (+diencephalon, +striatum) (B2) III,IV (limbic) (C2) moderate(6–19 neuritic plaques/1 mm2)
(A3) 4 (+brainstem),5 (+cerebellum, +pons) (B3) V,VI (neocortical) (C3) frequent(>20 neuritic plaques/1 mm2)

The ABC score is a good indicator for the likelihood of dementia.

Example: Cerebellar abeta deposits (A3) + tangles in entorhinal cortex and few temporal (B2), + 15 neuritic plaques per 1 mm2 (C2) -> (A3, B3, C2): intermediate AD level change.

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.

Prion diseases

General

Etiology:[40]

  • Misfolded cell-surface protein called PrPSC.
    • This is derived from the protein PrPC encoded by the PRNP gene.
  • Different genetics strains are associated with varying clinical phenotype.[41]


Includes:

  • Creutzfeldt-Jakob disease (CJD).
  • Sporadic fatal insomnia (sFI).[40]
  • Fatal familial insomnia (FFI).[42][43]
  • Gestmann-Straussler-Scheinker syndrome (GSS) - due to PRNP gene mutations.[44]

IHC

PrPC:[42]

  • Congo red +ve.
  • PAS +ve.

Creutzfeldt-Jakob disease

  • Commonly abbreviated as CJD.

General

  • Rare.
  • Incurable disease.

Usually diagnosed clinically:

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

Variant Creutzfeldt-Jakob disease

  • Abbreviated vCJD.
General
  • Associated with bovine spongiform encephalopathy (AKA mad cow disease).
  • Should sample: spleen, lymph nodes, tonsils.[45]

Microscopic

Features:

  • Spongy appearance (cytoplasmic vacuolization[46]).

Note:

Molecular

  • The CJD phenotype is associated with a PRNP D178N mutation and valine polymorphism at codon 129 (D178N-129V).
    • Note: A Met129 polymorphism will cause Fatal familiar insomnia in the setting of the same PRNP D178N mutation. [48]


Alpha-synucleinopathies

Without clincial information Parkinson's disease and Dementia with Lewy bodies cannot separated in histology.

Dementia with Lewy bodies

General

Clinical features:

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

Microscopic

Features:

Note: Cortical Lewy bodies are easily missed in HE.

IHC

  • Alpha-synuclein +ve.

Images

Parkinson disease

General

  • Common - often sporadic.
  • May be genetic.

Clinical TRAP:[49]

  • Tremor.
  • Rigidity.
  • Akinesia.
  • Postural instability.

Genetics:[50]

  • LRRK2 gene[51] - autosomal dominant.
  • PARK2 gene (parkin)[52] - autosomal recessive.

Gross

Features:[53]

  • Abnormally pale substantia nigra.
    • Pigmentation increases with age.
  • Pale locus ceruleus.

Notes:

Microscopic

Features:[53]

  • Loss of pigmented (catecholaminergic) neurons in the substantia nigra and locus ceruleus.
  • Gliosis - due to neuron loss.
  • Lewy bodies (in remaining neurons) - key feature.
    • Eosinophilic cytoplasmic inclusion with "dense" (darker) core and pale (surrounding) halo.
      • Consist of filaments composed of alpha-synuclein.
  • Lewy neurites - alpha-synuclein positive processes.

IHC

  • Alpha-synuclein +ve.

Images

Molecular

  • Hereditary forms in less than 10% of the cases
    • Involved genes are consecutively labeled PARK1, PARK2....

Multiple system atrophy

Multiple system atrophy is a neurodegenerative disease of the parkinsonism-plus disorder group.

General

Clinical findings variable:

  • Parkinsonism (stiatonigral degeneration, MSA-P).
  • Ataxia (olivo-ponto-cerebellar degeneration, MSA-C).
  • Autonomic dysfunction (Shy-Drager syndrome, depreceated).
  • Clinical onset between 40-60 years.
  • Progedient tremor, atxia, laryngeal paresis, wakness, cognitive decline.
  • Patients usually succumb after 6 years from aspiration pneumonia.

DDx:

Macroscopy

Microscopic

Features:

  • Inclusions cerebral, subcortical white matter, cerebellar.
  • Neuronal loss and gliosis (absent in minimal-change MSA).
  • Alpha-synuclein-rich glial and neuronal cytoplasmic inclusions in white matter (finding at autopsy).[54]
    • Inclusions in oligodendrocytes (triangular, flame-like or sickle-shaped) are definitive diagnostic for MSA.[55][56]
    • Inclusions usu. abundant in basal ganglia, substantia nigra, pontine nuclei, medulla and cerebellum.
  • Pons and Putamen:
    • Nuclear inclusions (sparse in most cases).
    • Neuropil threads (alpha-synuclein).
  • Loss of myelinated fibers from external capsule, striatum and pallidum.

Images

Molecular

  • No known alpha-synuclein mutation.
  • Genetic variants of SNCA gene assoicated with MSA. [57]

Tauopathies

More than 20 different degenerative disorders can be classified as tauopathies.[58] FTLD-tau is an umbrella term used for tauopathies including PSP, CBD, PiD and GGT. [59]


Argyrophilic grain disease

Corticobasal degeneration

  • AKA CBD.
  • Symptoms may vary:
    • Progressive asymmetrical rigidity and apraxia, progressive aphasia or dementia.
  • Neuronal and glial Tau-positive inclusions.[60]
    • Astrocytic plaques.
    • Thread-like lesions and coiled bodies.
    • Ballooned neurons +/-.
  • Pathology is cortical and striatal and Gallyas-positive.
  • Neuronal loss in the substantia nigra.

DD: PSP (widespread neurofibrillary degeneration, with characteristic globose NFT).

Globular glial tauopathies

  • Commonly abbreviated GGT.
  • AKA sporadic multiple system tauopathy.
  • Rare disease.[61]
  • Combination of frontotemporal dementia and motor neuron disease or only part thereof.
  • 4-repeat tauopathy.

Microscopic

  • Globular oligodendroglial and astrocytic Tau inclusions.
  • Absence of tufted astrocytes.
  • Mostly Gallyas-negative.


Progressive supranuclear palsy

  • Commonly abbreviated PSP.
  • AKA Steele-Richardson-Olszewski syndrome.

General

  • Diagnosis - clinical.[62]

Clinical:

  • Impaired control of gaze, esp. difficulty looking up and down (supranuclear palsy).[63]
  • Parkinsonism.[15]

Microscopic

Features:[1][62][64]

  • 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.[65][66]

Images:

Pick disease

General

  • Dementia.

Gross

  • Frontal and temporal lobe atrophy.[67]
    • May be called "walnut brain"[68] - as it resembles a walnut.

Microscopic

Features:[67]

  • Pick cells = large ballooned neurons.
  • Pick bodies = round, homogenous, intracytoplasmic inclusions, size ~10 micrometers.

Image(s):

TDP Proteinopathies

FTLD-TDP

  • Accounts for about 50% of all FTLD cases.
  • Degeneration of frontal and temporal lobes.
  • Inclusions not seen in HE or silver stains.
  • TDP43-positive
    • Neuronal cytoplasmic inclusions.
    • Neuronal intranuclear inclusions.
    • Dystrophic neurites.
  • Ubiquitin+ve.
  • p62+ve.
  • aSynculein-ve.
  • Tau-ve.
  • FUS-ve.
  • Four FTLD-TDP subtypes
    • Type A: compact nuclear/cytoplasmatic inclusions, associated with GRN mutations.
    • Type B: diffuse nuclear/cytoplasmatic inclusions most often seen in C9orf72 expansion.
    • Type C: dystrophic neurites.
    • Type D: Lentiform nuclear inclusions, only in cases with VCP mutations.
  • C9orf72 mutated show additional DPR+ve staining of TDP‐43‐ve inclusions.
    • These addtional inclusions are ubiquitin+ve and p62+ve

FTLD-FET

  • Clinical manifestations depend on the distribution of the pathologic alterations in the CNS
  • Currently 3 disorders among the FTLD-FET subgroup.
  • In contrast to ALS-FUS, no genetic alterations of FUS have been reported to date for cases within the FTLD-FUS group.
  • 5–10% of all FTLD cases
  • Deposited Proteins: FUS, EWS, TAF-15.
  • FUS‐positive inclusions in FTLD cases show co‐aggregation of TAF15 and EWS
    • (Different from ALS-FUS)

DDx (also FUS+ve):

  • Spinocerebellar Ataxia (SCA)
  • Huntington Disease (SD)


Atypical FTLD‐U

  • Early onset frontotemporal dementia, rapidly progressive psycho‐behavioural changes.
  • Neuronal cytoplasmic inclusions in hippocampus and frontotemporal lobes.
  • Ubiquitin+ve, tau/TDP‐ve.
  • FET+ve inclusions
    • Unique vermiform filamentous neuronal nuclear inclusions.
  • Caudate nucleus head degeneration and hippocampal sclerosis.

Basophilic inclusion body disease

  • AKA: BIBD.
  • Variable clinic (behavioral, cognitive alterations, parkinsonism, motor neuron diseases, ALS-like).
  • Age of onset: 35-70 years.
  • Intraneuronal cytoplasmic basophilic inclusion bodies.
  • FUS+ve (universally).
  • EWS+ve.
  • TAF15+ve.
  • alpha-Internexin+ve.

Neuronal Intermediate Filament Inclusion Disease

  • AKA: NIFID.
  • Sporadic early‐onset frontotemporal dementia, motor neuron disease, extrapyramidal motor symptoms.
  • Hyaline conglomerates (brightly eosinophilic branching fibrillar structures embedded in a round, well-delineated, glassy vacuole).
  • Deposits in cerebral cortex, hippocampus, basal ganglia, thalamus, cerebellar dentate, numerous brainstem nuclei and lower motor neurons.
  • FUS+ve/EWS+ve/TAF15+ve (heterogenous).
    • FET+ve filamentous nuclear inclusions in the hippocampus.
  • Ubiquitin +/-ve.
  • NF +ve (some subunits).
  • p62 +/-ve.
  • TDP43-ve.
  • Tau-ve.
  • α-synuclein-ve.

Other

Chronic traumatic encephalopathy

  • Abbreviated CTE.

Huntington disease

General

  • Autosomal dominant inheritance.
  • Mutation in Huntington gene (HTT):[70]
    • 11-34 CAG repeat = normal.[71]
    • >42 CAG repeat = Huntington disease.

Clinical:[72]

  • Early onset dementia.
  • Involuntary movements (chorea) - both arms and legs.
  • Behaviour changes, e.g. grimacing.
  • Speech changes.

Gross

  • Severe caudate atrophy.[73]
    • Prominent frontal horns of the lateral ventricles.[74]

Note:

  • A normal caudate bulges into the ventricle.

Images:

Microscopic

Features:[72]

  • Neuron loss.
  • Gliosis.

Binswanger 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.

Frontotemporal lobar degeneration with ubiquitinated inclusions

Abbreviated FTLD with ubiquitinated inclusions or FTLD-TDP43.

General

  • There are several forms of frontotemporal dementia.
  • Related to amyotrophic lateral sclerosis (ALS); also a TDP-43 pathology.[75]
    • There are several subtypes of FTLD with TDP-43.

Gross

  • Frontal and temporal lobe atrophy.

Image:

Amyotrophic lateral sclerosis

  • Abbreviated ALS.

General

  • AKA Lou Gehrig's disease.
  • Characterized by motor neuron death.
  • May be familial and associated with C9orf72 expansion, or SOD1, FUS and TARDBP mutations.[76][77]
  • Pathological protein aggregates cause dysfunction of RNA-binding proteins.

Clinical

  • Peak incidence: 50-60yrs.
  • 2-5 per 100,000 individuals worldwide.
  • Dead after disease onset: Usu. 2-5yrs.
  • Weakness (Progressive bulbar, limb, thoracic, and abdominal muscle atrophy).
  • About 20% of ALS cases develop frontotemporal lobar degeneration (FTLD).
  • Environmental toxins are discussed (Guam ALS).[78]

Microscopic

Features:[76][79]

  • Loss of the giant cells of Betz.
  • Motor neurons with eosinophilic inclusions (Bunina bodies).
    • PAS positive cytoplasmic inclusions.
  • Motor neuron loss + reactive gliosis + neurogenic muscular atrophy.
    • Loss of myelinated axons in the lateral and anterior columns of the spinal cord.
  • Ubiquitinated cytoplasmic inclusions.[80]
  • TDP-43 proteinopathy in motor neurons (90% of all sporadic ALS cases).
  • C9orf72 expansion cases: p62+ve, TDP-43-ve inclusions in the dentate gyrus, neocortex, and cerebellum.[82]
    • FUS-mutant cases show FUS+ve, p62+ve (few) and TDP-43-ve inclusions.[83]

Images:

DDx:

  • Spinal muscular atrophy.
  • Primary Lateral Sclerosis.
  • Hereditary Spastic Paraparesis (HSP).

Hallervorden-Spatz disease

  • AKA pantothenate kinase-associated neurodegeneration.

General

  • Uncommon.

Microscopic

Features:[85]

  • Axonal spheroids.
  • Iron deposition.

Images:

Stains

  • Prussian blue +ve.

See also

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