FTD Turkish characte..

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Frontotemporal Frontotemporal lobar lobar degeneration: degeneration: demographic and clinical demographic and clinical characteristics characteristics in a Turkish dementia population in a Turkish dementia population Görsev G. Yener Görsev G. Yener , M.D. , M.D. Neurology Neurology , Dokuz Eylül University , Dokuz Eylül University Izmir, Turkey Izmir, Turkey [email protected] [email protected]

Transcript of FTD Turkish characte..

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Frontotemporal Frontotemporal lobar degeneration: lobar degeneration: demographic and clinical characteristics demographic and clinical characteristics

in a Turkish dementia populationin a Turkish dementia population

Görsev G. YenerGörsev G. Yener, M.D., M.D.

NeurologyNeurology, Dokuz Eylül University, Dokuz Eylül University

Izmir, TurkeyIzmir, Turkey

[email protected]@deu.edu.tr

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FTLD FTLD Prevalence Prevalence

Not clearNot clear ( (4-4-16%)16%)

Common cause pre-senile dementiaCommon cause pre-senile dementia

1:1 with AD 45-64 year1:1 with AD 45-64 yearss (Ratnavalli Neurology 2002)(Ratnavalli Neurology 2002)

more common than AD below 60 years more common than AD below 60 years (Knopman Neurology 2004)(Knopman Neurology 2004)

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FTLDFTLD in Izmir, Turkey in Izmir, Turkey

Demographic Demographic datadata

GeneticsGenetics//Pathological Syndrome Pathological Syndrome

Neary Criteria – FTD, PA, SDNeary Criteria – FTD, PA, SD

MND associationMND association

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1994-2004 Izmir DEU Dementia Clinic1994-2004 Izmir DEU Dementia Clinic

N=1169 N=1169

Demented= 66 % Demented= 66 %

AD (possible / probable) 67 % AD (possible / probable) 67 %

Vascular dementia 15 % Vascular dementia 15 %

Fronto-temporal dementia 4 %Fronto-temporal dementia 4 %

Lewy body dementia 9 %Lewy body dementia 9 %

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FTLD Clinical Heterogeneity

Genetic & sporadic casesGenetic & sporadic cases

Histology variesHistology varies

Motor overlap with PSP, CBD, ALSMotor overlap with PSP, CBD, ALS

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Neary CriteriaNeary Criteria Frontotemporal Lobar DegenerationFrontotemporal Lobar Degeneration

Frontotemporal DementiaFrontotemporal Dementia

Progressive Non-Fluent AphasiaProgressive Non-Fluent Aphasia

Semantic DementiaSemantic Dementia

Neary et al. 1998, NeurologyNeary et al. 1998, Neurology

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Dokuz Eylül University Dokuz Eylül University Dementia and Movement Disorders ClinicsDementia and Movement Disorders Clinics

1994-20011994-2001

35 FTLD, 25 PSP, 5 CBD cases35 FTLD, 25 PSP, 5 CBD cases

Demographic and clinical featuresDemographic and clinical features

WebsterWebster

MMSE (subitems)MMSE (subitems)

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FTLD: GenderFTLD: Gender

****

TurkishTurkish (N=35) (N=35) (% male)(% male)

Ag

e (

Years

)A

ge (

Years

) ****

39%40%

72%

59%

0

20

40

60

80

FTD SD PNFA MND

40%

67%64%

0

20

40

60

80

FTD SD PNFA

USUS (N=353) (N=353) (% male)(% male)

Johnson et al. Johnson et al. Arch NeurolArch Neurol. 2005;62:925-930.. 2005;62:925-930. Yener et al 2002Yener et al 2002

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FTLD: Age at OnsetFTLD: Age at Onset

****

5859

63

50

55

60

65

FTD SD PNFA

US (N=353US (N=353))

Ag

e (

Years

)A

ge (

Years

)

Johnson et al. Johnson et al. Arch NeurolArch Neurol. 2005;62:925-930.. 2005;62:925-930.

61

72

61

50

55

60

65

70

75

FTD SD PNFA

Turkish (N=35)Turkish (N=35)

?

Yener et al 2002Yener et al 2002

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Presenile onset (%) -TurkishPresenile onset (%) -Turkish

26%

100%

48%46%

0

20

40

60

80

100

**

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40-60 %40-60 %

In Netherland series 38% In Netherland series 38%

(15 million screened) (15 million screened)

Family Hx (+) , RR=3.5Family Hx (+) , RR=3.5

Family historyFamily history

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Family Hx (%)-Turkish population

10%

24%20%25%

54%

0

0

0

0

0

1

1

FTLD

(N=35

)

PSP (N

=25)

CBD

(N=5)

AD (N

=390)

VAD

(N=65

)

****

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FTFTLLD D PathologicalPathological Syndrome SyndromeCore FeaturesCore Features

Frontotemporal predominanceFrontotemporal predominance

Gliosis, spongiosus, neuronal lossGliosis, spongiosus, neuronal loss

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Variable Histological FeaturesVariable Histological FeaturesNeuronal inclusions with ubiquitinNeuronal inclusions with ubiquitin

(Clinical: MND, ALS, Paget, Inclusion body myositis)(Clinical: MND, ALS, Paget, Inclusion body myositis)

Neuronal inclusions Neuronal inclusions with tauwith tau (Clinical: FTDP-17, PSP, CBD)(Clinical: FTDP-17, PSP, CBD)

Other inclusionsOther inclusions (Neuronal intermediate filament inclusion dementia)(Neuronal intermediate filament inclusion dementia)

No inclusionsNo inclusions (DLDH) (DLDH) (Clinical: FTLD)(Clinical: FTLD)

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Pick Bodies Cerebral cortex(Described by Alzheimer in 1911)

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Time (minutes)

Dis

tanc

e tr

avel

led

by th

e ta

u sp

ecie

s (

m)

B.A.

c d

0

20

40

60

80

100

150 175 200 225 250

0N4R-EGFP0N4RpCIneo

0N4R-EGFP0N4R-untagged

Courtesy of Tim Hutton, Cambridge, UK

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Tau mutations

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Bigio, et al, 2004, J Neuropath Exp Neurol, 63(8): 801 811

Neuronal ubiquitinated intranuclear inclusions in familial and non-familial

FTD-MND associated with ALS

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FTD with ubiquitinated neuronal inclusions and visuospatial impairment

Meiner et al Neurology 2005;65:478–480

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Ubiquitin and TauUbiquitin and Tau

Ubiquitin is a marker for a given protein to Ubiquitin is a marker for a given protein to be sent to a proteasome for degradationbe sent to a proteasome for degradation

Ubiquitin proteins are also needed for the Ubiquitin proteins are also needed for the degradation of taudegradation of tau

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FTD Neuropathology SubtypesFTD Neuropathology Subtypes

FTD-Ub FTD-Ub related to MND subtyperelated to MND subtype

CBD, PSP major tau subtypeCBD, PSP major tau subtype

DLDH DLDH less common withless common with new stain new staining ing techniquestechniques

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Clinical FeaturesClinical Features

SubtypesSubtypes

MNDMND

ParkinsonismParkinsonism

MMSEMMSE

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FTLD subtypes in the US and TurkeyFTLD subtypes in the US and Turkey

PNFA (n=11)31%

SD (n=3)9%

FTD (n=21)60%

PNFA (n=87)25%

SD (n=66)19%FTD

(n=200)56%

Johnson et al. Johnson et al. Arch NeurolArch Neurol. 2005;62:925-930.. 2005;62:925-930.

3 sites (N=353)3 sites (N=353)

1 site (N=35)1 site (N=35)Yener et al 2002Yener et al 2002

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MND and FTDMND and FTD are associatedare associated

FTD is associated with MND (15%)FTD is associated with MND (15%)

Most Most ALS ALS patients developpatients develop FTD FTD

FTLD-ALSFTLD-ALS chr chr 9 9 andand 17 17

Hypometabolism in fHypometabolism in frontal rontal lobes in ALSlobes in ALS

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Chang et al, Neurology 2005;65:75–80

Brain atrophy in ALS and ALS/FTLD

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FTLD ; 78%

FTD_MND; 22%

0%

10%

20%

30%

40%

50%

60%

70%

80%

FTLD FTD_MND

Turkish FTLD and MND

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Webster scores-Turkish FTLD subtypesWebster scores-Turkish FTLD subtypes

4,4

0,51

0,6

0,00

1,00

2,00

3,00

4,00

5,00

6,00

7,00

8,00

FTD SD PNFA FTD-MND

Clinical Features-ParkinsonismClinical Features-Parkinsonism

**

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Clinical FeaturesClinical Features

Parkinsonism appears earlier in FTLDParkinsonism appears earlier in FTLD

MND - more often parkinsonismMND - more often parkinsonism

No tau mutation was found in FTD-MND group.No tau mutation was found in FTD-MND group.

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MMSE Scores in Turkish FTLDMMSE Scores in Turkish FTLD

14,1014,10

24,30 23,60

0

20

FTLD PSP CBD MND-FTD

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MMSE Figure copying (%)MMSE Figure copying (%)

63%

0%

69%

33%

0

20

40

60

80

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Clinical patternsClinical patterns

PSP~CBD PSP~CBD

Both higher Webster and MMSE Both higher Webster and MMSE scoresscores

MMSE figure copy is discriminativeMMSE figure copy is discriminative

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Clinical patternsClinical patterns

Webster scores Webster scores FTD-MND > FTLDFTD-MND > FTLD

MMSE scoresMMSE scores FTD-MND = FTLDFTD-MND = FTLD

preserved figure copying preserved figure copying FTD-MND > FTLDFTD-MND > FTLD

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Clinical patternsClinical patterns

FTLD subtypes FTLD subtypes

total MMSE total MMSE PNFA < PNFA < SDSD < FTD < FTD

figure copyfigure copy SDSD < PNFA < FTD < PNFA < FTD

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ConclusionsConclusions FTLDFTLD common in presenile ages common in presenile ages

Turkish Turkish FTLD FTLD subtypes have similar subtypes have similar profile to the USprofile to the US

FTD> PNFA > SD FTD> PNFA > SD

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ConclusionsConclusions Higher family Hx than other dementias Higher family Hx than other dementias

(54%)(54%)

FTLD-MND association (22%)FTLD-MND association (22%)

FTD-MND has higher parkinsonism FTD-MND has higher parkinsonism scores scores