ATYPICAL PARKINSONISM GUIDE

ATYPICAL PARKINSONISM
DR.SARATH MENON.R, MD(Med.),DNB(Med.),MNAMS
DM RESIDENT
DEPT. OF NEUROSCIENCES
AIMS,KOCHI

OUTLINE
 Classifications
 Red flag signs
 AP- syndromic approach
 Diagnostic criteria
 Phenotypic spectrum
 Atypical AP or mimickers
 Investigations
 Novel biomarkers
 Treatment
 Future trends

INTRODUCTION
 Common problem in neurology outpatient
departments
 Wide variety of sporadic / heredodegenerative
syndromes
 Aetiologies vary widely
 80-85% -IPD
 Differentiation from other syndromes
 Very important in prognostication and management

AKINETIC RIGID SYNDROMES -
CLASSIFICATION
 Primary (Idiopathic) Parkinsonism
 Multisystem Degenerations
 . Heredodegenerative Parkinsonism
 Secondary (Acquired, symptomatic) Parkinsonism

 Primary Parkinsonism Parkinson’s Disease
 - Sporadic Parkinson’s Disease
 - Hereditary

MULTISYSTEM DEGENERATIONS
(PARKINSONISM PLUS)
 Progressive Supranuclear Palsy
 Multiple System Atrophy (Shy-Dragger syn.) SND
(MSA P)
OPCA (MSA C)
 Corticobasal Degeneration
 Diffuse Lewy Body Disease
 Lytico-Bodig disease (Parkinsonism Dementia ALS
-Complex of Guam)
 Progressive pallidal Atrophy
 Parkinsonism dementia Complex
 Pallido pyramidal Degenerations

HEREDO DEGENERATIVE
 Hereditary Juvenile Dystonia Parkinsonism (AR Parkin
Mutation)
 Dopa - Responsive Dystonia
 Huntington’s Disease
 Wilson’s Disease
 Hereditary Ceruloplasmin Deficiency
 Frontotemporal dementia with parkinsonism
 Mitochondrial Cytopathies with Striatal Necrosis
 PKAN (Neurodegeneration associated with brain Iron
accumulation; Hallervorden - Spatz Disease)

 Spinocerebellar Degenerations (Eg: MJD)
 Gerstmann - Straussler - Scheinker Disease
 Familial Progressive Subcortical Gliosis
 Familial Basal Ganglia Calcification
 Lubag(X Linked dystonia - Parkinsonism)
 Ceroid Lipofuscinosis
 Neuroacanthocytosis
 Hereditary Haemochromatosis.
 Neuroferritinopathy
 Aceruloplasminemia

SECONDARY PARKINSONISM
 Infectious Post- encephalitic
 HIV; SSPE; Prion diseases
 Drugs
 Dopamine Receptor Blocking drugs, Reserpine, Tetrabenazine, Alpha
Methyl Dopa, Lithium, Flunarizine, Cinnarizine.
 Toxins
 MPTP, Carbon monoxide, Manganese, Mercury, Carbon
disulfide,Cyanide, Methanol.
 Vascular -Multi infarct; Binswangers disease.
 Trauma -Pugilistic Encephalopathy.
 Parathyroid abnormalities;
 Hypothyroidism;
 Brain Tumors
 Paraneoplastic
 NPH
 Psychogenic.

IDIOPATHIC PD
 UK Brain Bank Criteria
 bradykinesia and at least one of the following: rest
tremor, rigidity, or postural instability.

RED FLAGS
 Symmetric bradykinesia and rigidity
 Absence of tremor
 Prominent myoclonus
 Limb apraxia
 Alien limb phenomena
 Impaired down gaze
 Facial dystonia
 Early loss of postural reflexes
 L- dopa induced facial dyskinesias
 Ataxia
 Stridor
 Early dysphagia
 Spasticity
 Early dementia or hallucinations
 Early and prominent dysautonomia

MAJOR SYNDROMES
 PSP
 MSA
 CBGD
 DLBD

PATHOPHYSIOLOGY
 Accurate diagnosis is necessary to understand
pathogenesis
 Two proteins mainly
 Alpha synuclein
- Pre synaptic protein
- Aggregates in cell body & neurons – lewy body &
lewy neuritis- PD & DLBD
- glial cytoplasmic inclusion in MSA

TAUPATHY
 4 repeat tau accumalates
 NFT & in glia
 Psp- astrocytic tufts
 CBD- astrocytic plaques

PROGRESSIVE SUPRANUCLEAR PALSY
 Steele et al—1964
 5% of parkinsonian pts
 Prevalence—4.9 / 100,000
 Incidence 1.7 (50-59yrs) to 14.7(80-89yrs)
 Commonly misdiagnosed as PD
 Insidious onset
 No pathologic proven cases have begun before the
age of 40.

 Tauopathy-4-repeat t, 4R tauopathy).
 always sporadic, few familial cases-
- MAPT (microtubuli associated protein t) gene mtn.
 Mitochondrial dysfunction & oxidative stress -
pathophysiology of PSP

Postural Instability & EP Features :
 Falls—backward
 Poor postural reflexes
 Rigidity –axial
 Dysarthria—spastic,
 Hypophonic
 ataxic
 Frontal release signs
 Pseudobulbar palsy
 L-DOPA UNRESPONSIVENESS

 Reduced blink rate and closure of eyelids due to eyelid
dystonia or levator inhibition ( apraxia of eyelid
opening)
 square wave-jerks
 on doll’s eye maneuver, there is improved range, as
vestibulo-ocular reflex is preserved
 Subcortical-type dementia
 Typical facies- “surprised look”

NINDS–SPSP DIAGNOSTIC CRITERIA FOR PSP
 Possible PSP
Mandatory inclusion criteria:
 gradually progressive disorder
 onset age 40 or later
 Either vertical supranuclear palsy or both slowing of
vertical saccades
 postural instability with falls within a year of disease onset
 no evidence of other diseases that could explain the
foregoing features, as indicated by exclusion criteria

Mandatory exclusion criteria:
 recent history of encephalitis
 alien limb syndrome
 cortical sensory deficits
 focal frontal or temporoparietal atrophy
 hallucinations or delusions unrelated to
dopaminergic therapy
 cortical dementia of Alzheimer type
 prominent, early cerebellar symptoms
 unexplained dysautonomia

Supportive features:
 symmetrical akinesia or rigidity
 proximal more than distal
 abnormal neck posture
 especially retrocollis
 poor or absent response of parkinsonism to levodopa
 early dysphagia and dysarthria
 early onset of cognitive impairment including two or
more of: apathy, impairment in abstract thought,
decreased verbal fluency, utilisation or imitation
behaviour, or frontal release signs

Probable PSP
Mandatory inclusion criteria
 gradually progressive disorder
 onset age 40 or later
 vertical supranuclear palsy
 prominent postural instability with falls within a year
of disease onset
 no evidence of other diseases that could explain
the foregoing features, as indicated by exclusion
criteria

Definite PSP
Mandatory inclusion criteria:
 clinically probable or possible PSP and
histopathological evidence of typical PSP

PHENOTYPIC SPECTRUM OF PROGRESSIVE
SUPRANUCLEAR PALSY
 typical PSP phenotype- Richardson syndrome
 PSP-p = PD at least at the initial stages, with asymmetric
parkinsonism, rest-tremor, better levodopa response, longer
mean survival
 pure akinesia with gait freezing (PSP-PAGF)
 corticobasal syndrome (PSP-CBS),
 frontotemporal dementia (PSP-FTD), progressive nonfluent
aphasia
 no clinical sign to predict PSP pathologic abnormality
accurately in the non-RS phenotypes

INVESTIGATIONS
 clinical diagnosis
 MRI-
midbrain atrophy
Superior cerebellar peduncle atrophy.
“morning glory flower sign” and the “hummingbird sign” are
quite specific but show low sensitivity (50% and 68.4%,
respectively
 (DATscan) is abnormal in PD and all AP syndromes

 differentiate with PD, [123]meta-iodobenzylguanidine
(MIBG) and 123I-iodobenzamide (IBZM) SPECT may be
useful
 MIBG is abnormal in PD because of postganglionic
sympathetic denervation, but is typically normal in PSP.
 IBZM SPECT assessing the postsynaptic receptors is
abnormal in PSP and normal in PD
 IBZM SPECT is abnormal in all APs and therefore
cannot differentiate between PSP and other AP
 Novel diagnostic approaches and biomarkers
- csf tau protein
-neurofilament light chain

PATHOLOGY
 Neurofibrillary tangles are present in these areas.
 Tufted astrocytes (Gallyas-positive) -hallmark
feature of PSP that differentiates other 4R
tauopathies such as CBD (astrocytic plaques

RX
 no effective symptomatic or neuroprotective treatments
 A trial of levodopa (up to 1 g/d) and amantadine (up to 450 mg/d)
 Botulinum toxin injections can be used to treat levator inhibition.
 Serotonin reuptake inhibitors (SSRIs) may be used for apathy with no
clear benefit.
 A small study with Coenzyme Q10- no RCT study
 Recent large, double-blind studies with GSK-3b inhibitors (Tideglusib,
Davunetide) have failed to show any clinical effect.
 Tideglusib reduced the rate of brain atrophy in one study.
 Supportive measures such as physiotherapy, walking aids, speech
therapy and PEG

MULTIPLE SYSTEM ATROPHY :
 Sporadic neurodegenerative disorder clinically any
combination of parkinsonian, autonomic, cerebellar, or
pyramidal signs
 Pathologically–
cell loss, gliosis, and glial cytoplasmic inclusions in
several CNS structures.
 MSA is an a-synucleinopathy
 usually a sporadic disease; however, rarely, familial
cases - mutations in COQ2 gene

 Epidemiology :
 prevalence of MSA in four studies ranged from 1·9
to 4·9 cases per 100 000 people.
 similar to those of other well-known
neurodegenerative disorders such as Huntington’s
disease and motor neuron disease.
 no single environmental factor shown to increase
or to reduce risks of MSA

Clinical presentation :
 affects both men and women
 the sixth decade of life progresses with a mean
survival of 6–9 years.
 substantial variation of disease progression with
survival of more than 15 yrs.
main features –
 autonomic failure
 Parkinsonism
 cerebellar ataxia
 pyramidal signs in any combination.

TWO MAJOR MOTOR PRESENTATIONS
 distinguished clinically–
 Parkinsonian features predominate in 80% of
patients (MSA-P subtype),
 cerebellar ataxia is the main motor feature in 20%
of patients (MSA-C subtype).
 Both similar survival times.
 patients with MSA-P have a more rapid functional
deterioration than those with MSA-C

 MSA-P-associated parkinsonism :
 progressive akinesia and rigidity
 jerky postural tremor and tremor at rest.
 orofacial or craniocervical dystonia associated with a
characteristic quivering high-pitched dysarthria.
 Postural stability is compromised early on in the
disease course
 recurrent falls at disease onset are unusual in
contrast to psp.

 90% of the MSA-P pts- unresponsive to levodopa in
the long term.
 50% have levodopa-induced dyskinesia affecting
orofacial and neck muscles, without motor benefit.
 fully developed clinical picture of MSA-P evolves
within 5 years of disease onset, allowing a clinical
diagnosis during follow-up.

MSA –P RED FLAGS
 Early instability
 Rapid progression
 Pisa syndrome,camptocormia,contractures
 Bulbar dysfunction
 Respiratory dysfn- stridor,insp sighs
 Emotional incontinence
 2/6 – probable MSA-P – additional criteria

MSA-C :
 gait ataxia
 limb kinetic ataxia
 scanning dysarthria,
 cerebellar oculomotor disturbances.
 Most patients develop additional non-cerebellar
symptoms and signs
 may be indistinguishable from other patients with
idiopathic late onset cerebellar ataxia

 Dysautonomia :
 urogenital and orthostatic dysfunction.
 Early erectile dysfunction is nearly universal in men
with MSA
 Female- genital insensitivity
 urinary incontinence or retention are common early
in the course or as presenting symptoms

CONSENSUS STATEMENT FOR THE CLINICAL
DIAGNOSIS OF MSA
 clinical domains,
 features
 criteria used in the diagnosis of MSA

 Autonomic and urinary dysfunction :
 Features
 1. Orthostatic hypotension
 2. Urinary incontinence or incomplete bladder emptying
Criteria
 Reduction of least 30mmHg or in diastolic blood pressure
by at least 15 mm Hg after 3 min of standing
 urinary incontinence (persistent, involuntary partial or
total bladder emptying, accompanied by erectile
dysfunction in men) or both

 Parkinsonism :
 A. Features
 1. Bradykinesia
 2. Rigidity
 3. Postural instability (not caused by primary visual,
vestibular, cerebellar, or proprioceptive dysfunction) 4.
Tremor (postural, resting or both)
 B. Criteria
 Bradykinesia plus at least one of features 2–4

 Cerebellar dysfunction :
 A. Features
 1. Gait ataxia
 2. Ataxic dysarthria
 3. Limb ataxia
 4. Sustained gaze-evoked nystagmus
 Criteria
 Gait ataxia plus at least one of features 2–4

 Corticospinal tract dysfunction
 A. Features
 1. Extensor plantar responses with hyper-reflexia
 Criteria
 Corticospinal tract dysfunction in MSA: no
corticospinal tract features are used in defining the
diagnosis of MSA
 prominent and severe spasticity should raise
suspicion for an alternative diagnosis

Consensus statement: exclusion criteria for the
diagnosis of MSA :
 History
 Symptomatic onset under 30 years of age
 Family history of a similar disorder
 Systemic disease or other identifiable causes
 Hallucinations unrelated to medication
 DSM IV criteria for dementia
 Prominent slowing of vertical saccades or vertical
supranuclear gaze palsy
 Evidence of focal cortical dysfunction such as aphasia,
alien limb syndrome, and parietal dysfunction
 Laboratory investigation- Metabolic, molecular genetic
and imaging evidence of an alternative cause of
features

DIAGNOSTIC CLINICAL APPROACH
Motor signs
 Parkinsonism poorly responsive to levodopa
 Cerebellar ataxia
 Pyramidal signs
 Early instability and falls Within 3 years of disease
onset
 Rapid progression (wheelchair sign) despite
dopaminergic treatment within 5 years of disease
onset

 Orofacial dystonia or dyskinesias
 Atypical spontaneous or levodopa induced
dystonia
 dyskinesia mainly affecting orofacial muscles,
[resembling risus sardonicus of cephalic tetanus]
 Axial dystonia -Pisa syndrome (subacute axial
dystonia with a severe tonic lateral flexion of the
trunk, head, and neck)
 early severe camptocormia
 Disproportionate antecollis -Chin on chest, neck
can only be passively and forcibly extended to its
normal position with difficulty; despite severe
chronic neck flexion, flexion elsewhere is minor.

 Jerky tremor
 Irregular myoclonic postural or action tremor of the hands
or fingers
 Dysarthria-
- Atypical quivering, irregular and severely hypophonic or
slurring high pitched dysarthria,
- tends to develop earlier and be more severe than in PD
 notable dysphagia

Non-motor signs
 Severe dysautonomia
 Abnormal respiration
 Nocturnal (harsh or strained, high pitched inspiratory
sounds) or diurnal inspiratory stridor,
 involuntary deep inspiratory sighs and gasps, sleep
apnoea
 snoring increased from premorbid level
 newly arisen REM sleep behaviour disorder

“RED FLAGS’’
 RBD and autonomic failure- pre motor stage
 Early falls and postural instability can be seen- look for
eye signs & fronto-subcortical dysfunction for PSP
 L-dopa induced oro facial dystonia- MSA
 Raynaud phenomenon is a common in MSA
 Freezing of gait may be prominent, early, and severe,
causing diagnostic difficulties -PSP -PAGF phenotype
 dementia, it is considered a non supporting feature for
the diagnosis of MSA
 frank, prominent, early dementia should lead the clinician
to other diagnoses.

Investigations
 Autonomic function tests
 Cardiovascular function test-within in 2-3 ys
 Bladder function tests
 standard urine analysis will exclude infection.
 The residual volume –usg,cystometry ,UDS

IMAGING
 MRI
- Hot cross burn sign- mcp/pons- MSA-c
- Putaminal rim- MSA-p
- DAT scan
- abnormal in all MSA, PSP, and PD
- MIBG scintigraphy
- abnormal in PD, normal in MSA
 IBZM SPECT is normal in PD,abnormal in MSA (but
also in PSP and CBD)

NOVEL BIOMARKERS
 Mollenhauer and colleagues-
CSF mean a-synuclein levels , not total t, or Ab42 levels
differentiated PD and MSA from neurologic controls (70%
sensitivity, 53% specificity)
 a-synuclein and phosphorylated t/total t could differentiate
PD from MSA -sensitivity of 90% & specificity of 71%
 Flt3 ligand, a cytokine
PD and MSA with a sensitivity of 99% and a specificity of
95%.

RX
 Symptomatic
 PD- L-dopa/ dopa agonists- cranio cervical dystonia
postural hypotension
Amantidine- gait disturbances
 Orthostatic hypotension-
high salt, fludrocortisone,midodrine
 Urinary dysfunction
- UDS- characterise nature
-Neurogenic bladder- Oxybutinin or Tolderotidne
 Erectile dysfunction-
- sildenafil
-intracavernosal inj. Or penile implants

- SSRI/TCA
RCT – Rasagiline and rifampicin- no effects
Promising studies
- IVIG
- Intrarterial/IV autologous stem cells
- Future
- Alpha synuclein targeting antibodies

CORTICOBASAL DEGENERATION :
sixth to eighth decades of life,
onset of symptoms at mean age 63 years (SD 7·7)
. sporadic disease
4–6% of parkinsonism,

Clinical presentations
 Five initial presentations
 The most common presentation (55%) -“useless
arm” (ie, a rigid, dystonic, akinetic, or apraxic arm),
 gait disorder (27%)
 prominent sensory symptoms
 isolated speech disturbance
 behavioural disturbance

 Clinical features
Motor
Limb clumsiness (asymmetric)
Bradykinesia/Akinesia (asymmetric)
Rigidity (asymmetric)
Tremor (action/postural)
Myoclonus
Limb dystonia (asymmetric)
Blepharospasm
Choreoathetoid movements
Speech abnormalities
Gait disorder

Higher cortical functions
 Apraxia (limb more common than orofacial, eyelid-
opening)
 Dementia
 Alien-limb phenomenon
 Aphasia
 Frontal-lobe-release signs
 Cortical sensory abnormalities
 Depression
 apathy
 Anxiety Irritability
 Disinhibition
 Delusions
 Obsessive compulsive disorder

DIAGNOSTIC CRITERIA FOR CORTICOBASAL
DEGENERATION
Inclusion criteria (one of A or B)
A) Rigidity (easily detectable without reinforcement) and
one cortical sign:
 apraxia (more than simple use of limb as object;
absence of cognitive or motor deficit sufficient to explain
disturbance)
 cortical sensory loss (preserved primary sensation,
asymmetric)
 alien-limb phenomenon (more than simple levitation)
B) Asymmetric rigidity, dystonia (focal in limb; present at
rest at onset),
 focal reflex myoclonus (spreads beyond stimulated digits

Exclusion criteria
 Early dementia (will exclude some patients with
corticobasal degeneration)
 Early vertical gaze palsy
 Rest tremor
 Severe autonomic disturbances
 Sustained responsiveness to levodopa
 Lesions on imaging studies indicate another
pathological process

PROPOSED CRITERIA FOR THE DIAGNOSIS OF
CORTICOBASAL DEGENERATION
Core features
 Insidious onset and progressive course
 No identifiable cause (eg, tumour, infarct)
 EPS – one of the follow
-focal or asymmetric appendicular rigidity
-lacking prominent and sustained l-dopa response
-focal or asymmetric appendicular dystonia
 Cortical dysfunction - at least one of the following
: focal or asymmetric ideomotor apraxia
alien-limb phenomena
cortical sensory loss visual or sensory hemineglect
constructional apraxia
focal or asymmetric myoclonus
apraxia of speech or nonfluent aphasia

Supportive investigations
 Variable degrees of focal or lateralised cognitive
dysfunction,
 with relative preservation of learning and memory
on neuropsychometric testing
 Focal or asymmetric atrophy on CT or MRI imaging,
typically in perifrontal cortex
 Focal or asymmetric hypoperfusion on SPECT or
PET, typically maximal in parietofrontal cortex with
or without basal ganglia involvement

NEUROPATHOLOGICAL CRITERIA
Core features
 Focal cortical neuronal loss
 Substantia nigra neuronal loss
 Cortical and striatal Gallyas/tau-positive neuronal and
glial lesions, especially astrocytic plaques and threads, in
both white and grey matter
Supportive features
 Cortical atrophy, commonly with superficial spongiosis
 Ballooned neurons, in atrophic cortices
 Tau-positive oligodendroglial coiled bodies

PHENOTYPIC SPECTRUM OF CORTICOBASAL
DEGENERATION
 Classic CBD phenotype- CBS
 CBD- present with FTD,RS,PPA,PCA
 AD,PSP,FTD present with CBS
 Symmetrical bilateral CBS- AD pathology/RS
 Early onset PSP – CBD pathology
 For which proposed clinical criteria applied

INVESTIGATIONS
 Imaging
asymmetric frontal, and parietal cortical atrophy becomes
evident with dilatation of the lateral ventricle
 EEG –
-normal at first
- show asymmetric slowing that is maximum over the
hemisphere contralateral to the more affected limb
 Dopamine transporter SPECT- abnormal
- differentiate them from those with Alzheimer’s and Pick’s
diseases (in whom this scan is typically normal) early in
the course of the disease.

 FDG-PET
- Asymmetric reduction in fronto parietal regions

RX
 Anecdotal
 L-dopa trial (upto 1 gm/d)/Amantadine- PD symptoms
 Valproate, Levetiracetam- myoclonus
 Botox inj- dystonic hand
 No trials with ACEI – dementia
 Palliative rx

“CORTICO BASAL DEGENERATION-LOOKALIKE”
SYNDROMES
 atypical manifestations of PSP
 -progressive nonfluent aphasia FTD.
 Parkinson’s disease
 multiple-system atrophy
 Wilson’s disease
 progressive subcortical gliosis
 rigid-akinetic type Huntington’s disease
 atypical Pick’s disease
 parkinsonism– dementia–amyotrophic-lateral-sclerosis
complex
 prion related disease
 sudanophilic leukodystrophy
 neurofilament inclusion disease.

DEMENTIA WITH LEWY BODIES
Central feature (essential for a diagnosis of possible
or probable DLB)
 Dementia -progressive cognitive decline of sufficient
magnitude to interfere with normal social or
occupational function.
 Prominent or persistent memory impairmen- not occur
in the early stages ,usually evident with progression.
 Deficits on tests of attention, executive function, and
visuospatial ability may be especially prominent.

CORE FEATURES (TWO CORE FEATURES ARE SUFFICIENT FOR
A DIAGNOSIS OF PROBABLE DLB, ONE FOR POSSIBLE DLB)
 Fluctuating cognition with pronounced variations in
attention and alertness
 Recurrent visual hallucinations that are typically well
formed and detailed
 Spontaneous features of parkinsonism

SUGGESTIVE FEATURES
 REM sleep behavior disorder
 Severe neuroleptic sensitivity
 Low dopamine transporter uptake in basal ganglia
demonstrated by SPECT or PET imaging
 (If one or more of these is present in the presence of one
or more core features, - probable DLB .
 In the absence of any core features, one or more
suggestive features is sufficient for possible DLB.
 Probable DLB should not be diagnosed on the basis of
suggestive features alone.)

SUPPORTIVE FEATURES (COMMONLY PRESENT BUT NOT
PROVEN TO HAVE DIAGNOSTIC SPECIFICITY)
 Repeated falls and syncope
 Transient, unexplained loss of consciousness
 Severe autonomic dysfunction, e.g., orthostatic hypotension, urinary
incontinence
 Hallucinations in other modalities
 Systematized delusions
 Depression
 Relative preservation of medial temporal lobe structures on CT/MRI
scan
 Generalized low uptake on SPECT/PET perfusion scan with reduced
occipital activity
 Abnormal (low uptake) MIBG myocardial scintigraphy
 Prominent slow wave activity on EEG with temporal lobe transient
sharp waves

A DIAGNOSIS OF DLB IS LESS LIKELY
 If -CVA evident as focal neurologic signs or on brain
imaging
 In the presence of any other physical illness or brain
disorder sufficient to account in part or in total for the
clinical picture
 If parkinsonism only appears for the first time at a stage
of severe dementia

TEMPORAL SEQUENCE OF SYMPTOMS
 diagnosed when dementia occurs before or concurrently
with parkinsonism (if it is present).
 Parkinson disease dementia (PDD) - dementia that occurs
in the context of well-established Parkinson disease.
 In research studies in which distinction needs to be made
between DLB and PDD, the existing 1-year rule between
the onset of dementia and parkinsonism - DLB continues
to be recommended.

CLINICAL MANAGEMENT
 Motor parkinsonism-
-Levodopa at low doses & titrate up.
-Anticholinergics should be avoided.
 Neuropsychiatric symptoms.--cholinesterase inhibitors
(CHEIs) or atypical antipsychotic

“ATYPICAL” ATYPICAL PARKINSONISM
 Misdiagnosis PD with AP , as well as FTD,AD,PPA
 Mimickers of Atypical PD
Eg:
SCAS/ FTAX- mimic MSA
Neimann Pick C,CTX,prion d/s,mitochondrial- mimic AP
phenotype
- Age of onset
- Tempo of progression
- Family history
- Clinical exam + associated features

SUMMARY
 Careful clinical examination
 Expanding phenotypic spectrum of AP & expanding
pathological spectrum of classic AP phenotypes –
diagnostic challenge
 AP mimickers
 Investigations may be supportive, but their sensitivity
and specificity are low.
 There are currently no biomarkers available.
 There are currently no neuroprotective treatments
available.
 symptomatic and supportive treatments with usually no
sustained effect.
 Further research required

ATYPICAL PARKINSONISM GUIDE

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