The Predictivity Concept

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The Predictivity Concept Peter Propping Institute of Human Genetics University of Bonn, Germany CDBI Seminar on predictivity, genetic tests and insurance Strasbourg, 3-4 December 2007

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The Predictivity Concept. Peter Propping Institute of Human Genetics University of Bonn, Germany. CDBI Seminar on predictivity, genetic tests and insurance Strasbourg, 3-4 December 2007. Heart disease. PKU. Schizophrenia. Motor vehicle accident. Cancer. Multiple sclerosis. - PowerPoint PPT Presentation

Transcript of The Predictivity Concept

Page 1: The Predictivity Concept

The Predictivity Concept

Peter ProppingInstitute of Human Genetics

University of Bonn, Germany

CDBI Seminar on predictivity, genetic tests and insurance

Strasbourg, 3-4 December 2007

Page 2: The Predictivity Concept

Source: Dr. Ron Zimmern, Oxford

Gene-environment Interaction:

Cystic fibrosis

Fragile XDuchenne muscular dystrophy

Heart disease

PKU

Cancer

Diabetes

Multiple sclerosis

Schizophrenia

Asthma TBObesity

Alzheimer

Autism

MeningococcusStruck

bylightning

Motor vehicle

accident

Rheumatoid arthritis

‘Totally’ Genetic

‘Totally’Environmental

Page 3: The Predictivity Concept

The Human Genome

3,2 x 109 nucleotide pairs

not a “unique” sequence, but appreciable interindividual variation

any two genomes: 99,9% DNA sequence identity,

thus, 0.1 % sequence differences (3 mio).Any individual (diploid, i. e. two genomes):6 mio differences to the reference genome.

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Modes of inheritance

?

Autosomal dominant

?

Autosomal recessive

?

X-chromosomal

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Two major groups of genetic diseases

Monogenic (= Mendelian) disorders

- monocausal

- clear relationship between genotype and phenotype

- about 2.000 disorders clarified

- most disorders are rare

- therapy mostly difficult

Genetically complex (multifactorial) disorders

- complicated genetic structure

- many of them common in the population

- may be influenced by exogenous factors

- therapy frequently possible

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Conceptual distinction

- Prognosis: statement about the future course of a past

or currently existing disorder

- Prediction: probability of the onset of a disease

that has not yet occurred

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Methods of prediction and prognosis in a proband

- medical history

- medical examinations

- family history

- predictive genetic diagnosis

- prediction based on lifestyle

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Prediction on the basis of medical examinations

Imaging techniques (CT, MRT, Ultrasound)- e.g. polycystic kidney disease

hereditary brain tumors, e.g. tuberous sclerosisdegenerative brain disorders

Electrocardiogram- e.g. hereditary disturbance of conductivity (long QT-syndrome)

Blood biochemistry- e.g. hypercholesterolemia

hyperlipidemia

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I:1

60 y

I:2

58 y

II:1

36 y

II:2

34 y

II:4

21 y

II:3

34 y

III:1

10 y

III:2

8 y

III:3

5 y

Genetic diagnostics in familial adenomatous polyposis (FAP)

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I:1

60 y

I:2

58 y

II:1

36 y

II:2

34 y

II:4

21 y

II:3

34 y

III:1

10 y

III:2

8 y

III:3

5 y

Predictive diagnostics in familial adenomatous polyposis (FAP)

Page 11: The Predictivity Concept

CRC, 56y

CRC, 32yHNPCC?

30y 28y

? ?

2y

Persons at risk for Lynch Syndrome

(Hereditary Nonpolyposis Colorectal Cancer, HNPCC)

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Cumulative risk in carriers of amutation in the BRCA1 or BRCA2 gene

Meta-analysis, King et al., Science 2003

BRCA1 BrCa

BRCA2 BrCa

BRCA1 OvCa

BRCA2 OvCa

Gen.pop. BrCa

Gen.pop. OvCa

X

0

10

20

30

40

50

60

70

80

90

100

0 30 40 50 60 70 80

X

X

XXX

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Examples for Hereditary disorders with late onset for which predictive genetic diagnosis is possible (autosomal-dominant)

Treatable:Hereditary tumor syndromes:- breast/ovarian cancer- colorectal cancer- familial adenomatous polyposisPolycystic kidney disease, type 1Hereditary deafness, several late onset forms

Untreatable:Huntington diseaseMyotonic dystrophyAlzheimer disease, autosomal-dominant formsSpinocerebellar ataxia, several formsFacio-scapulo-humeral muscular dystrophyRetinitis pigmentosa, several late onset forms

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Concordance rates in identical (monozygotic, MZ) and fraternal (dizygotic, DZ) twins

%

MZ DZ

Coronary heart disease 46 12

Hyperthyroidism 47 7

Neurodermitis 83 28

Diabetes mellitus I 45 5

Diabetes mellitus II 95 10

Lepra 59 20

Epilepsy („idiopathic“) 86 4

Schizophrenia – narrow definition 26 4-10

– wide definition 41 10-20

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Genetic model of a complex (multifactorial) disease:

Hypertension as an example

„„super-normal“super-normal“ slightly slightly predisposedpredisposed

slightly slightly increased increased

definitely definitely increasedincreased

severely illseverely ill

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Relationship between genotype and phenotype in a complex disease

- Predictive value of a genotype

• Positive Predictive Value (PPV)

- Fraction of persons with a predisposing genotype who will develop the disease

• Negative Predictive Value (NPV)

- Fraction of persons without the genotype who do not have the disease

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Positive Predictive Value (PPV):

Example: Crohn disease and association with NOD2 variant

NOD2 Genotype Patients Controls

Wildtype / Wildtype 227 248

Wildtype / Ins 57 23

Ins / Ins 20 1

Positive predictive value:

Homozygous 20 = 0,95

Heterozygous 57 = 0,71

2021

5780

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Relationship between Genotype Frequency, Relative Risk and Positive Predictive Value

Disease Disease Genotype Genotype Relative Risk PPVFrequency Frequency

COPD+ 0,05 Pi ZZ 0,0005 20,0 99,1%

Narcolepsy 0,0005 DQB1*0602 0,021 10,5 0,4%homozygosity

+COPD = chronic obstructive pulmonary disease

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Predictability of affection status in the carrier of a predisposing genotype

- monogenic diseases

• up to 100% depending on penetrance

- complex (multifactorial) diseases

• often low

• eventually higher after genotypic profiling

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To what degree can multifactorial

disorders be predicted ?

Generally, the concordance rate of MZ twins is the upper limit of prediction;

but: only cross-sectional information taken into account, no age correction possible;

global concordance rates give only average data, in fact part of the cases higher degrees of heritability may exist.

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Screening approaches:

- Genetic population screening

• newborn screening for treatable diseases

• e. g. preconceptual thalassemia screening on Sardinia and Cyprus

• preconceptual screening in certain ethnic groups, e. g. for Tay-Sachs in Jews

• cascade screening, e. g. for hypercholesterolemia in the Netherlands

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Screening approaches:

- Ascertainment of persons at high risk through family history

• e. g. inherited breast/ovary cancer and Lynch syndrome (HNPCC)

• population-based for preconceptual testing in recessive diseases

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The Future:

The “1000 Dollar Genome”

- nightmare of informed consent

- nightmare of interpretation