Jana Povova, Omar Sery, Hana Tomaskova, Petr Ambroz,
Anna Pohlidalova, Vladimir Janout
Department of Epidemiology and Public Health, Ostrava, Czech Republic
Department of Biochemistry, Brno, Czech Republic
EPIDEMIOLOGY AND GENETICS OF ALZHEIMER´S
DISEASE
INTRODUCTION It is generally accepted that Alzheimer´s disease It is generally accepted that Alzheimer´s disease
(AD) is the most frequent form of dementia.(AD) is the most frequent form of dementia. Etiology of AD is still unknown and there are Etiology of AD is still unknown and there are
three hypotheses, what risk factors are three hypotheses, what risk factors are responsible for development of the disease:responsible for development of the disease:
- vascular risk factors- vascular risk factors
- genetic risk factors- genetic risk factors
- behavioral risk factors- behavioral risk factors
EPIDEMIOLOGY From different reasons there are no exact data From different reasons there are no exact data
about the incidence and prevalence of ADabout the incidence and prevalence of AD
- no compulsory notification- no compulsory notification
- difficult to distinguish between different- difficult to distinguish between different
forms of dementiaforms of dementia
- no exact diagnostic test- no exact diagnostic test There are mostly only estimates of real There are mostly only estimates of real
incidence or prevalence … in the Czech incidence or prevalence … in the Czech Republic 120 000 cases of AD notifiedRepublic 120 000 cases of AD notified
STUDY
Since 2010 we have been performing an Since 2010 we have been performing an epidemiological study to assess the importance epidemiological study to assess the importance of selected risk factors from vascular and of selected risk factors from vascular and genetic fields.genetic fields.
The aim of the study is to recruit 800 cases of The aim of the study is to recruit 800 cases of AD and 800 controls.AD and 800 controls.
In this paper we report some preliminary results In this paper we report some preliminary results from analyses of 394 cases and 287 controls.from analyses of 394 cases and 287 controls.
DIAGNOSTIC CRITERIA
CASES
- MMSE < 24
- slow development of cognitive impairment
- other forms of dementia excluded (CT exam.)
CONTROLS
- MMSE > 28
- same gender and age (± 5 years)
EPIDEMIOLOGICAL DATA
Recruitment: 394 Cases 130 Controls Gender: 79 % females 76 % females Age (average) 79 73 96,7 % of cases with late onset (after 65 years) Education: in group of cases 49 % elementary,72 %
lower than high school
in group of controls 36 % high school Clinical course: in 85 % slow
SELECTED VASCULAR RISK FACTORS
RISK FACTOR
cases controls
OR95% CI p-value
% %
CVD 52 % 43 % 1,44 0,94-2,19 0,089
Diabetes 29 % 38 % 0,67 0,44-1,02 0,062
Hypertension 69 % 79 % 0,57 0,36-0,92 0,022
Stroke 15 % 22 % 0,63 0,38-1,04 0,069
Head Injury 4 % 6 % 0,69 0,29-1,64 0,403
GENETICS We start with focusing on genes:
- Apolipoprotein E (ApoE)
- Angiotensin Converting Enzyme (ACE) Gene for ApoE is found on chromosome 19q13.2
and has 3 major alleles 2,3,4.• It has 6 genotypes depending on combination of
these three alleles.• The allele 4 is the only confirmed genetic factor
contributing to both early and late onset of AD.
GENETICS
ACE gene is located on the chromosome 17q23 and has 2 major alleles I and D.
• It has 3 genotypes depending on combination of these two alleles.
• It was reported that the ID and II genotypes are associated with the risk of AD (DD genotype is considered as neuroprotective).
Apolipoprotein E (ApoE)
ApoE4 allele significantly increase the risk of AD. (OR 2,52; 95% CI 1,832-3,482)
In both files the genotype E3/E3 was most frequent (cases 47 % and controls 60 %)
The frequency of genotype E4/E4 was in cases 3 %, in controls 0,3 % only.
E2 E3 E4
patients (n=373) 5,23 70,64 24,13
controls (n=286) 10,49 78,32 11,19
OR 0,47 0,66 2,52(95% CI) X X (1,832-3,482)
Frequency of apolipoprotein alleles %
Frequency of apolipoprotein E genotypes (%)
E2/E2 E2/E3 E3/E3 E2/E4 E3/E4 E4/E4patients (n=373) 0,27 6,97 47,45 2,95 39,41 2,95controls (n=286) 0,70 17,48 59,80 2,09 19,58 0,35
OR X X X 1,41 2,67 8,66
(95% CI)X X X
0,51 – 3,88 1,86 – 3,82 1,11 – 67,48
p-valueX X X
0,62 ˂0,0000 0,01
Genotypes ACE
Allele I increases risk of AD (OR 1,08; 95% CI 0,87 – 1,34) but so far difference is not significant.
In both files the genotype ID was most frequent – cases 49 % and controls 57 %.
Genotype II was in cases in 22 % and in controls in 17 % (marginal significant difference – OR 1,43 95% CI 0,97-2,12)
Frequency of I, D alleles (%)
I D
patients (n=384) 47,14 52,86
controls (n=287) 45,12 54,88OR 1,08 0,92
(95% Cl) 0,87 – 1,34 0,74 – 1,14
p-value 0,472 0,472
Frequency of genotypes (%)
II ID DDpatients (n=384) 22,39 49,48 28,13controls (n=287) 16,72 56,79 26,49OR
1,43 0,75 1,09(95% CI) 0,97-2,12 0,54-1,01 0,77-1,53
Conclusions – vascular risk factors
In patients with AD were CVD more often in their history compare to controls but the difference was not significant.
Diabetes, stroke and hypertension were inversely related to AD what is contrary to some published results.
In case of hypertension the inversal difference was statisticaly significant. The same finding was published by some other researchers.
Conclusions – genetic risk factors
Relationship between ApoE4 allele and AD was confirmed in presented paper with high statistical significance, what make it possible diagnostic marker for AD.
In ACE gene was only marginal reliance of alelle I presence and higher risk of AD development.
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