PHARMACOGENETICS

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PHARMACOGENETICS

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Title: PHARMACOGENETICS

1
PHARMACOGENETICS

XENIA GONDA
Department of Pharmacology and Pharmacotherapy
Department of Clinical and Theoretical Mental
Health
Semmelweis University

New field within clinical pharmacology (30-40
years)
Patients respond differently to a given
therapeutic agent even if they have the same
illness
The same dose of a given drug in some patients
causes very different plasma levels and different
therapeutic response

3
Pharmacogenetics

The study of
genetically determined
interindividual differences in
therapeutic response to drugs and
susceptibility to adverse effects (Lerer)

4
History

510 BC Pythagoras some people develop haemolytic
anaemia after eating fava beans
1902 Garrod genetic factors direct chemical
transformations
1932 Snyder phenylthiourea nontasting is
inherited as an autosomal recessive trait
1957 Motulsky first demonstration of the
relationship between adverse drug reaction and
genetically determined variation
1959 Vogel pharmacogenetics the hereditary
basis of variability in drug effects
1960 Evans speed of INH acetylation is under
genetic control
1962 Kalow abnormal form of serum cholinesterase
causes adverse reactions to succinylcholine
1977 Mahgoub polymorphism of CYP2D6 causes
adverse effects to debrisoquine
Lerer

5
Aim of pharmacogenetic studies

Identify and categorize the genetic factors that
underlie the differences and apply this in
clinical practice
Rational, individual therapy
Screening for those patients who carry the genes
which place them at risk in case of certain
therapies
Discovering which drugs are potentially dangerous
for carriers of a given polymorphism
Establishing the frequency of pharmacogenetic
phenotypes

Pharmacogenetics study of genetically determined
interindividual differences in response to drugs
Pharmacogenomics use of genome based techniques
in drug development
The differences in the response to a given drug
can be attributed to two major factors that are
under genetic influence
Pharmacokinetic genetically based differences in
the processes influencing bioavailability
Pharmacodynamic genetically based differences in
the proteins at which the drug acts

7
Polymorphism

Genetic variation occuring with a frequency of 1
or more in the population
1. SNP (single nucleotide polymorphism)
most frequent type
difference in a single base of the genomic
sequence
usually 1/1000 base
most does not influence the structure or function
of proteins
SNP can occur
In exons (may alter the structure of proteins and
may lead to functional consequences)
In introns (may influence splicing)
In the regulatory regions (may influence
expression of the gene)

8
Polymorphism II

2. Insertion/deletion polymorphism insertion or
deletion of a few nucleotides
3. Variable number tandem repeats variation in
the number of times a sequence of several hundred
base pairs is repeated
4. Simple tandem repeats (microsatellites) 2-4
nucleotides repeated a variable number of times

9
Polymorphism III

Pharmacogenetic traits are mainly
polygenic (influenced by several genes, the
effect may be additive or interactive)
multifactorial (both genetic and environmental
factors contribute)
Some pharmacogenetic traits are
monogenic

Genotype gene structure encoding for the given
characteristics
Phenotype the manifestation of the genotype,
which can be observed and can be influenced by
other factors
Other gene products
Environment
Acquired characteristics
Frequency of genetic polymorphisms differs
greatly among ethnic groups
The functional relevance of a given polymorphism
can vary across ethnic groups

Determination of genotype PCR
Determination of phenotype
determination of metabolic rate (level of
original drug/metabolit in urine)
after administration of a given dose of the drug,
pharmacokinetic parameters are measured
(halflife, clearance, plasma levels)
Distribution of phenotypes in the population
Multimodal (usually bi- or trimodal) distribution
indicates determination by a single gene having
polymorphic variants
Unimodal distribution indicates polygenic
multifactorial inharitance, or monogeic
inheritance but no polymorphism

The function is usually bi- or trimodal
indicating two or three phenotypes
Enhanced/extensive metaboliser
intensive metabolisation, resulting in low plasma
concentration of the drug
usually heteozygote or homozygote dominant
Intermedier metaboliser
Poor metaboliser or nonmetaboliser
Slow or no metabolisation of the drug resulting
in high plasma concentration for an extended time
Usually homozygote recessive

13
Types of adverse effects of drug therapy
14

The observed differences in therapeutic response
and and susceptibility to adverse reíctions are
due to alterations of pharmacokinetic and
pharmacodynamic processes
Absorption
Distribution
Protein binding
ACTION
METABOLISM
Disposition

15
Inheritance of the activity of metabolic enzymes

Monogenic inheritance
one gene is responsible for encoding the enzyme
mutant enzyme variants may cause defects in
metabolism, leading to different genotypes within
the population
usually autosomal recessive in case of the allele
carrying the reduced enzyme function
Polygenic inheritance
several genes are responsible for encoding the
enzyme

16
Pharmacogenetics of drug metabolism

Drug metabolism is crucial in determining
therapeutic and adverse effects
Genetic factors play an important role in
individual differences of drug metabolism
Phase I
Oxidation, reduction, hydroxilation,
dealkylation, etc.
Aim introduce a new functional group
Cytochrome P450 enzymes in hepatocytes attached
to SER
Phase II
Conjugation with glucuronic acide, glutathione,
acetate, etc
Aim to increase water solubility
Ususally in the cytosol

17
Polymorphism of phase I metabolism

Cytochrome P450 enzyme polymorphisms
Sample reactions
Debrisoquine ? 4-OH-debrisoquine CYP2D6
Dextrometorphan ? dextorphan CYP2D6
Dextrometorphan ? methoxymorphinan CYP3A
Sparteine ? 2-dehydrosparteine CYP2D6
Mephenytoin ? 4-hydroxy-mephenytoin CYP2C9

Nomenclature of CYP genes
Arabic number for gene family
Capital letter for gene subfamily
Arabic number for individual gene
CYP enzymes of different gene families have a 40
or more homology in their amino acid sequences,
but enzymes within one subfamily may have
different substrates, regulation, etc.
Over 70 of total CYP content of the human liver
is shared by seven subfamilies CYP1A2, CYP2A6,
CYP2B6, CYP2C, CYP2D6, CYP2E1, CYP3A
Extent of metabolism is determined by
Affinity of substrate-enzyme complex
Relative abundance of a given CYP enzyme relative
to the total CYP content

19
CYP2D6

Discovered in the 1970s, one of the most widely
studied polymorphisms in drug metabolism
2 of total liver CYP content
Distribuiton of PM 7 of Caucasians, 1 of
Asians
Involved in metabolism of several drugs
Psychotropic medications tricyclic
antidepressants, SSRIs, classical and atypical
antipsychotics
Cardiovascular drugs
?-receptor antagonists metoprolol, propranolol,
timolol
Phenacetine
D-penicillamine
Codeine
Abused drugs

20
CYP2D6

More than 50 alleles, encoding enzymes with
inactive / decreased / increased / normal
catalytic function, up to a 1000fold variation in
the population
Poor metabolisers
are at risk of drug toxicity even at standard
doses, resulting in poor compliance
may also present with treatment resistance to
prodrugs that require activation (codeine)
Ultrarapid metabolisers
delayed therapeutic response or treatment
resistance (29 of Ethiopians carry multiplicated
functional CYP2D6 alleles)
Also present in brain functionally associated
with dopamine transporter, might have a role in
dopaminergic transmission, there are differences
in presonality traits between PMs and Ems

21
Distribution of CYP2D6 enzymes in different
populations
Ingelman-Sundberg et al., 1999
22
CYP2D6 polymorphism of debrisoquine metabolism

Debrisoquine is the most frequently used test
substrate in studies of the polymorphism of drug
metabolism
Frequency of phenotypes

23
CYP1A2 nonpolymorphic drug metabolism with
polygenic control

13 of total liver CYP content
Varies up to 130fold in individuals and in
populations
Important in disposition of several important
psychotropic medications clozapine, olanzapine

24
Polymorphism of phase II metabolism conjugation
I.

Paracetamol conjugated with glucuronide (55-60)
and sulphate (35), can be used for testing of
polymorphism of phase II reactions
UDPGT uridinglucuronyltransferase
PST sulphotransferase, both under monogenic
control, genetic deficiency is important in
Parkinsons disease, Gilbert syndrome,
Crigler-Najjar syndrome

25
Polymorphism of phase II metabolism conjugation
II.

Acetylation
INH (isoniazid) is acetylated by
N-acetyltransferase (NAT)
Speed of acetylation is genetically determined
bimodal distribution, slow and fast acetylators
Autosomal recessive inheritance
The rate of slow acetylators increases with age
Rate of slow acetylators is higher Gilbert
syndrome, rheumatoid arthritis, ischaemic heart
disease
N-substituted arylamines are less carcinogenic
after acetylations

26
Frequency of fast acetylators in different
populations
27
Other important pharmacogenetic polymorphisms I.

Glucose-6-phosphate dehydrogenase
Most frequent pharmacogenetic enzymopathy
130 enzym variants, only some are abnormal
Antimalaria drugs (primaquine), antibiotics
(sulfonamides, chloramphenicol, nitrofurantoine),
other medicines (quinine, quinidine,
phenylhydrazine, dapson) cause fatal haemolysis
in some patients
Favism haemolysis after consumption of legumes,
gooseberry, blackcurrant

28
Other important pharmacogenetic polymorphisms II.

Alcohol dehydrogenase (ADH)
Speed of ethanol?? acetaldehyde reaction is
increased
Acetaldehyde dehydrogenase activity is
unaffected, so acetaldehyde is not metabolised at
a sufficient rate
Acetaldehyde is accumulated causing flushing and
tachycardia
Frequency 5-20 in caucasians, 90 among Chinese

29
Other important pharmacogenetic polymorphisms
III.

Serum cholinesterase
Activity of serum cholinesterase is reduced in
some people (1/25000)
Administration of succinylcholine causes
paralysis of breathing muscles

30
Gene-environment interactions intraindividual
variability I.

Diet may alter hepatic cytochrome P 450 activity
Smoked foods (polycyclic aromatic hydrocarbons)
increase CYP1A activity (Kall Clausen 1995)
Cruciferous vegetables (brussels sprouts,
cabbage, broccoli) alter activity of selected
CYP isoenzymes
Indole-containing vegetables (cabbage,
cauliflower) upregulate CYP1A (Pantuck et al.,
1989)
Isothyocyanate-containing vegetables (watercress)
inhibit CYP2E1 (Kim Wilkinson 1996)
Organosulfur compounds (garlic) inhibit CYP2E1
and induce CYP1A, CYP3A and phase II enzymes
Grapefruit juice phytochemicals influence CYP3A
activity
Vitamins, spices

31
Gene-environment interactions intraindividual
variability II.

Drug-drug interactions
Enzyme inductors or inhibitors rifamycins,
anticonvulsants, macrolide antibiotics, azole
antifungal drugs, nefazodone, certain SSRIs
Nutraceutical influences herbs and dietary
compounds
St. Johns wort (Hypericum peforatum) CYP3A
inductor
Aging lower blood flow and liver volume
decreases from the third decade, but the effect
on enzymes is moderate
Disease
Acute inflammation and infection affect drug
metabolism
Liver disease modifies blood flow and reduces
enzyme activity

32
Cytochrome P450 isoenzymes involved in
polymorphism of drug metabolism
33
PSYCHOPHARMACOGENETICS
34
CYP enzymes important in psychiatry

CYP 1A2
Antidepressants amitryptiline, clomipramine,
imipramine, mirtazapine
Antipsychotics olanzapine
Beta blockers propranolol
Caffeine, paracetamol, theophylline, warfarine
CYP2C19
antidepressants citalopram, clomipramine,
imipramine
Barbiturates hexobarbithal, mefobarbithal
Beta blockers propranolol

35
CYP 2D6

Antipsychotics
haloperidol, terfenazine, risperidone,
thioridazine
SSRIs
fluoxetine, N-desmetilcitalopram, paroxetine
TCAs
amitryptiline, clomipramine, desipramine,
imipramine, nortryptiline
Other antidepressants
venlafaxine, nefazodone, trazodone, mirtazapine
Narcotics
codeine, dextrometorfane, etilmorphine
Antiarrhythmetics
encainide, flecainide, mexiletine, propafenone
Beta blockers
alprenolole, bufarolole, metoprolole,
propranolol, timolol

36
CYP 3A3/4

Antidepressants amitryptiline, clomipramine,
imipramine, nefazodone, sertraline,
o-desmetil-venlafaxine, mirtazapin
Antipsychotics clozapine
Benzodiazepines alprazolam, clonazepam,
diazepam, midazolam
Pain killers acetaminophen, alfentanyl, codein,
dextrometorphan
Antiarrhytmic drugs amiodarone, disopiramid,
lidocaine, propaphenon, kinidin
Ca antagonists diltiazem, felodipine,
nicardipine, nifedipine
Spasmolytics carbamazepine, ethosuximid
Antihistamines astemizole, rolatadine,
terfenadine
Anti-estrogens docetaxel, paclitaxel, tamoxifen
Macrolidos clarithromycine, erithromycine,
Steroidok androstendione, cortisol, estradiol,
ethynilestradiol, progesterone, testosterone,
dexamethasone
Other cisapride, dapson, lovastatine, omeprazol

37
PSYCHOPHARMACOGENETICS

Polymorphisms concerning the therpaeutic effect
of drugs influencing psychological functions
Primarily polymorphisms concerning the target
molecules of drug action (to a lesser extent
polymorphism of molecules involved in
pharmacokinetic processes)

38
Psychopharmacons

Drugs influencing the CNS functions and
psychological processes
Each neurotransmitter system regulates several
functions
A given drug binds to several target molecules
binding profile
In case of a given drug moluceule, target
molecule binding varies in different brain regions

39
Effect of psychopharmacons

Target molecules of drugs (receptors, enzymes,
transporters)
Key role in regulating neurotransmitter function
Directly or indirectly influence the development
of neural circuits and neuroplasticity
Quantity and function of gene products is
influenced by
Variations in gene structure (rare)
Variations in gene expression (more frequent)

Treatment response to antidepressant, anxiolytic
and antipsychotic drugs is influenced by genetic
factors
The genetic component is highly complex,
polygenic, epistatic (suppression of the effect
of a gene by a nonallelic gene)
Treatment response involves genetic and
environmental factors
Contribution of single genes to drug effect is
modest
Interaction between genes can result in a
dramatic modification of drug response additive,
nonadditive, synergistic

41
Serotonergic system

Mood
Cognition
Motor function
Circadian rhythms
Neuroendocrine system
Food intake
Sleep
Reproductive activity

42
Psychiatric disorders treatable with medications
acting through the serotonergic system

Depression
Anxiety
Impulse control disorders
Substance abuse
OCD
Somatic disorders, sexual disorders. Psychotic
disorders?

43
5-HTTLPR

SERT gene (SLC6A4) 17q11.1-q12

Lesch KP. (2001) J Affect Disord, 62 57-76.
44
The 5-HTTLPR polymorphism of the serotonin
transporter gene

17q11.1-q12
Promoter region
Insertion-deletion polymorphism
2 alleles s és l ? 3 genotypes ss, sl, ll
Functional polymorphism

45
Serotonin transporter and antidepressant response

Allelic variation in 5HTT function may lead to
Increased susceptibility to anxious and
depressive features
Less favourable antidepressant response in
patients affected by mood disorders

Smeraldi et al. 1998
Subjects carrying 5HTTLPR ll and ls genotypes
show better response for fluvoxamine than ss
subjects
Zanardi et al. 2000
Same results with paroxetine
Pollock et al 2000
ll patients display a faster response to
paroxetine
No difference in case of nortryptiline
(predominantly noradrenergic)
Whyte et al., 2001
Effect of 5HTTLPR on platelet activation in
geriatric depression

Rausch et al., 2002
Association between ll genotype and improved
response to fluoxetine
Significant increase in response to setraline in
eldery depressed ll patients
Former results might only apply to Caucasian
patients Korean and Japanese patients there is
a better response to fluoxetine, paroxetine and
fluvoxamine in ss patients

Benedetti et al., 1998
ll bipolar patients show superior mood
improvement after total sleep deprivation
Mundo et al., 2001
63 of patients with antidepressant induced mania
carried the s allele as compared to 29 in
bipolar subjects exposed to antidepressants not
developing mania
Michelon et al., 2006
Association between 5-HTTLPR genotype and
therapeutic response to lithium

49
Other important polymorphisms in
psychopharmacogenetics schizophrenia

D3 (Ser9Gly), D2 (Taq I és -141-C Ins/Del)
antipsychotic response, tardive dyskinesia
Adams et al. 2008 DRD3 and olanzapine response
in chronic scz
Sakumoto et al. 2007 DRD2 polymorphism predicts
response to DA antagonists in scz (bromberidol,
nemonaprid)
Kondo et al. 2003 DRD2 receptor polymophisms
predict treatment resistance in scz
5-HT2C (-759-T/C) antipsychotic treatment
related weight gain
(CYP2D6 ultrarapid metabolisers)

50
Other important polymorphisms in
psychopharmacogenetics depression

Choi et al. 2006 BDNF (Val66Met) polymorphism
and citalopram response
Domschke et al. 2008 MAO-A and antidepressant
response
Baune et al. 2008 COMT-A val158met amd
antidepressant response
Wilkie et al. 2008 HTR2A and paroxetine
treatment
Serretti et al., 2001 TPH1 slower response to
fluvoxamine
Schumann etal. 2001 DRD3 genotype and
antidepressive effect of sleep deprivation

51
Association between genetic polymorphisms and
drug effects