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Pharm 503
4th November 2019
Dalia A. Hamdy
BSc.(Pharm), MSc., PhD, RPh., MBA, MRSC
Founder and Manager of AbEx Health Services LTD.
Clinical Assistant Professor, FoPPS, University of Alberta
dhamdi@ualberta.ca
2-142K Katz
i. Getting introduced to the basics of
pharmacogenomics and its effect on drug
metabolism/pharmacokinetics (PK) and/or
pharmacodynamics (PK-PD).
ii. Apply Pharmacogenomics in precision medicine
iii. Having a Hands-on experience on the online
resources used to help you find dosing guidelines
(CPIC & PharmGKb)
iv. Integrating pharmacogenenomics into your clinical
assessment and decision in resolving drug therapy
problems and optimizing pharmacotherapy outcomes
Dr. Dalia A. Hamdy (FS 19/20AY) 2
1. Langman L, Dasgupta A. Pharmacogenomics in Clinical Therapeutics.;
Wiley-Blackwell 2012.
2. CPIC Guidelines for Simvastatin and SLCO1B1
https://www.pharmgkb.org/chemical/PA451363/guidelineAnnotation/
PA166105005
3. Roden D. Case Studies in personalized medicine. Vanderbilt University.
Online course through coursera.
https://www.coursera.org/lecture/personalizedmed/variability-in-drug-
therapy-spi4r
4. CPIC Guidelines for codeine and CYP2D6
https://www.pharmgkb.org/guidelineAnnotation/PA166104996
5. CPIC Guidelines for clopidogrel and CYP2C19
https://www.pharmgkb.org/guidelineAnnotation/PA166104948
6. CPIC Guidelines for voriconazole and CYP2C19
https://www.pharmgkb.org/chemical/PA10233/guidelineAnnotation/P
A166161537
7. Klein D. et al. PharmGKB summary: tamoxifen pathway,
pharmacokinetics. Pharmacogenet Genomics. 2013; 23(11): 643–647.
3Dr. Dalia A. Hamdy (FS 19/20AY)
1. SLCO1B1 is a (transporter/enzyme/receptor) that is
found in the hepatocytes also known as
(OATP1B1/OAT1B1/OCT1B1). The following Allelle(s)
(*1a/*5/*14/*2) has normal function whereas
(*1a/*5/*14/*2) has decreased function and
(*1a/*5/*14/*2) has increased function.
2. A patient shows up in your pharmacy with a genotype of
(*1a/*1a) what would be the recommended dose? Can we
give 80 mg qd for this patient? Why? What is your
reference?
3. A patient carrying a genotype of (*1a/*5) came across
your pharmacy and his cholesterol levels were not
adjusted using the 20 mg /day dose of statin? What would
be your recommendation?
4Dr. Dalia A. Hamdy (FS 19/20AY)
5Dr. Dalia A. Hamdy (FS 19/20AY)
6Dr. Dalia A. Hamdy (FS 19/20AY)
7Dr. Dalia A. Hamdy (FS 19/20AY)
8Dr. Dalia A. Hamdy (FS 19/20AY)
9Dr. Dalia A. Hamdy (FS 19/20AY)
“is the tailoring of medical treatment to the
individual characteristics of each patient”
The Age of Personalized Medicine
“The science of individualized prevention and
therapy”
National Institute of Health
10Dr. Dalia A. Hamdy (FS 19/20AY)
11
One Size fits all
medicine
Vs.
Personalized
medicine
Dr. Dalia A. Hamdy (FS 19/20AY)
12Dr. Dalia A. Hamdy (FS 19/20AY)
Pharmacogenetics:
The study of the effect of variations in DNA
sequence (genetic differences) on drug
response in terms of both the
metabolism/clearance (PK) and action (PD) of
the drug delivered
13Dr. Dalia A. Hamdy (FS 19/20AY)
14Dr. Dalia A. Hamdy (FS 19/20AY)
15Dr. Dalia A. Hamdy (FS 19/20AY)
1. What is DNA?
DNA (deoxyribonucleic acid),
 the cell’s hereditary material.
 DNA is a polymer of nucleotides
(sugar, phosphate and one of four
nitrogenous bases (A,T,G,C)
Human genome consists of
about 3.2 billion base pair (bp)
Every person has two copies of
each gene, one inherited from
each parent (6.4 billion bp)
DNA molecule is packaged into
thread-like structures called
chromosomes.
23 pairs of Chromosomes
 Sex chromosome XX or XY
 22 pairs autosomes
16Dr. Dalia A. Hamdy (FS 19/20AY)
2. What is the gene function?
DNA
• 99-98% Non-coding : its job is to actually regulate the
process whereby genes are translated into proteins.
• 1-2% coding : acts like the blueprint that encodes
proteins (enzymes, structural elements, signaling
molecules)
17Dr. Dalia A. Hamdy (FS 19/20AY)
3. Types of polymorphism
-SNPs (Single-Nucleotide Polymorphisms)
–Indels(Insertions & Deletions)
–VNTR (Variable Number Tandem Repeats)
–CNV (Copy Number Variants)
–Haplotypes (combination of alleles or to a set
of single nucleotide polymorphisms (SNPs) found
on the same chromosome
18Dr. Dalia A. Hamdy (FS 19/20AY)
 Gene mutations
 Inherited from a parent
 Acquired during a person’s lifetime
 Mutations range in size from
 single base-pair mutation that occurs at a
specific site in the DNA sequence (SNV)
 to a large segment of a chromosome (CNV)
19
SNP = SNV
which occur in
at least 1-2% of
the population
Dr. Dalia A. Hamdy (FS 19/20AY)
3. Types of genetic variants
SNP can be in the coding or non-coding regions
of the DNA resulting in
different proteins that could be functional or
non functional
20Dr. Dalia A. Hamdy (FS 19/20AY)
21Dr. Dalia A. Hamdy (FS 19/20AY)
• Polymorphism in enzymes, receptors and
transporters proteins can affect the PK and PD
of several medications
• In fact, 50–75% of medications are substrates of
the cytochrome P450 (CYP) 3A4 enzyme, 2C9,
and/or 2D6 metabolizing enzymes
• 50% of CPIC drugs guidelines involves 2C19, and/or
2D6
22Dr. Dalia A. Hamdy (FS 19/20AY)
23Dr. Dalia A. Hamdy (FS 19/20AY)
24Dr. Dalia A. Hamdy (FS 19/20AY)
Genes Alleles
CYP1A2 *1C, *1C, *1E,*1F, *1J, *1K, *1L, *1V, *1W, *6, *7, *8, *15
CYP2B6 *2, *4, *5, *6, *7, *8, *9, *13, *16, *18, *22, *34
CYP2C19 *2, *3, *4, *4B, *6, *8, *10, *17
CYP2C9 *2, *3, *4, *5, *6, *8, *9, *11, *12, *18, *27
CYP2D6 *2, *2A, *3, *4, *5, *6, *7, *9, *10, *14, *14A, *17, *29, *4N, *4M, *5, *6, *6C,
*7, *8, *9, *10, *11, *12, *13, *14A, *14B, *15, *17, *18, *19, *29, *31, *34, *35,
*36, *39,*41, *42, *63, *64, *68, *69, *70, *91, *109
CYP3A4 *1B, *3, *6, *11, *12, *16, *17, *18, *19, *22
CYP3A5 *2, *3A, *3B, *6, *7
COMT VAL158MET
DPYD *2A, *4, *5, *6, *9A, *13, rs7376798A
DRD2 PROMOTER VARIANT -241A>G
F2 20210G>A
F5 ARG534GLN (LEIDEN, 1691G>A)
GRIK4 NON-CODING (INTRONIC) T>C VARIANT
HTR2A INTRON 2, T>C VARIANT
HTR2C PROMOTER VARIANT -759C>T
IFNL3 rs1297860 C/T
IL28B (IFNL4) NON-CODING (INTRONIC) C>T VARIANT
NUDT15 ARG139CYS
OPRM1 ASN40ASP, A118G
SLC6A4 C,-1810A>G; -1791_-1749DEL43
SLCO1B1 *1B, *5, *9, *15, *31
TPMT *2, *3A, *3B, *3C, *4, *8
UGT1A1 *6, *27, *38, *60, *80
VKORC1 c.-1639G>T, A and G variants
25
Commercially available
pharmacogenomic testing
available in the Canadian
market
Dr. Dalia A. Hamdy (FS 19/20AY)
1. A patient appears with a T4 prescription in your pharmacy.
While discussing with him the use and checking his history you
realize that he has been on T3 and the pain is not manageable
and the dr. moved him to T4. In few days, he appears again
with a higher dose of codeine and still his pain is not in control.
-would you recommend a pharmacogenetic testing for this patient?
Why?
-If his PGX results came like that
CYP2D6 *4/*7, CYP2C19*1/*17, CYP2C9*1/*1, VKORC1 AA
What would you recommend and why?
2. What if the patient carried CYP2D6 *4/*9?
3. Knowing the mechanism of action of codeine, What other
information could be missing?
26Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
27Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
This had been determined using genotyping and
phenotyping. In phenotyping, a CYP2D6 specific probe
drug such as dextromethorphan is administered
the relative ratio between the concentration of probe
drug (dextromethorphan: DM) and its CYP2D6 specific
metabolite (dextorphan:DX)is obtained.
DM:DX ratios poor metabolizers.
DM:DX ratios extensive metabolizers
28Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
29Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
30Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
What is the effect of 2D6 on codeine?
Codeine
• Opiate analgesic
• Prodrug of morphine - is found naturally but
at low concentrations so usually synthesized
from morphine
31Dr. Dalia A. Hamdy (FS 19/20AY)
1. CYP 2D6
32Dr. Dalia A. Hamdy (FS 19/20AY)
33
1. Codeine is bioactivated to morphine, a strong opioid
agonist, by the hepatic cytochrome P450 2D6
2. The efficacy and safety of codeine are governed by
CYP2D6 activity.
3. Polymorphisms are a major cause of CYP2D6
variability.
Dr. Dalia A. Hamdy (FS 19/20AY)
Dr. Dalia A. Hamdy (SS18/19AY) 34
35
Similarly What about CYP2D6 and Tamoxifen?
Tamoxifen:
• a selective estrogen receptor modulator
• Used for the treatment and prevention of
estrogen receptor (ER)-positive breast cancer
• The drug is extensively metabolized by
CYP2D6 and other enzymes.
Dr. Dalia A. Hamdy (FS 19/20AY)
36Dr. Dalia A. Hamdy (FS 19/20AY)
37
Similarly What about CYP2D6 and Tamoxifen?
• 4-hydroxytamoxifen and endoxifen, are more
potent and considered the primary active
forms of the drug.
Dr. Dalia A. Hamdy (FS 19/20AY)
38
Phenotype Genotype Therapeutic
recommendation for
tamoxifen
Ultrarapid metabolizer More than two copies of
functional alleles
None
Intermediate metabolizer One active allele and one
inactive allele, or two
decreased activity alleles,
or one decreased activity
allele and one inactive
allele
Increased risk for relapse of
breast cancer. Avoid
concomitant use of CYP2D6
inhibitors. Consider
aromatase inhibitor for
postmenopausal women
Poor metabolizer Two inactive alleles Increased risk for relapse of
breast cancer. Consider
aromatase inhibitor for
postmenopausal women
Dr. Dalia A. Hamdy (FS 19/20AY)
39Dr. Dalia A. Hamdy (FS 19/20AY)
40Dr. Dalia A. Hamdy (FS 19/20AY)
41Dr. Dalia A. Hamdy (FS 19/20AY)
42Dr. Dalia A. Hamdy (FS 19/20AY)
43Dr. Dalia A. Hamdy (FS 19/20AY)
44Dr. Dalia A. Hamdy (FS 19/20AY)
45
PCI:Percutaneous coronary intervention
ACS: Acute coronary syndromeDr. Dalia A. Hamdy (FS 19/20AY)
46Dr. Dalia A. Hamdy (FS 19/20AY)
47Dr. Dalia A. Hamdy (FS 19/20AY)
48
1. What is expected to happen when I have
a. PM or IM CYP2C19?
b. UM or RM CYP2C19?
2. If we know that voriconazole is used for ttt
of invasive fungal infections in cancer patients.
Also that trough concentrations <2 mcg/ml is
associated with worse clinical outcomes? What
are the CPIC guidelines for a pt. with CYP2C19
*1/*17 or *2/*3?
Dr. Dalia A. Hamdy (FS 19/20AY)
49Dr. Dalia A. Hamdy (FS 19/20AY)
50Dr. Dalia A. Hamdy (FS 19/20AY)
51Dr. Dalia A. Hamdy (FS 19/20AY)
52
Using the CPIC guidelines how would you consider
carbamazepine therapy in the following pts.
1. A patient was using CBZ for 4 months and stopped
for problems with insurance coverage and
hospitalization periods. The dr. wants to restart him
again on CBZ. The dr. phones you and asks that he
heard about an available pharmacogenomic test
that is needed for this pt.? Would you strongly
recommend doing the test ? For what gene?
Why/why not?
2. The patient did the test and those were the results
CYP2D6 *4/*7, CYP2C19*1/*17, CYP2C9*1/*1, VKORC1
AA, HLA-B*15:02 negative
What would you suggest the dr. to do?
Dr. Dalia A. Hamdy (FS 19/20AY)
53
Using the CPIC guidelines how would you
consider carbamazepine therapy in the
following pts.
3. A naïve pt. patient wants to start CBZ
therapy and his genetic testing shows HLA-
A*31:01 genotype
What would you suggest the dr. to do?
Dr. Dalia A. Hamdy (FS 19/20AY)
54
Discussion point
Dr. Dalia A. Hamdy (FS 19/20AY)
Pharmacists are expected to
1. Be the point of testing for the patients
2. Receive the patients reports and interpret
them in a meeting in lay language
3. Keep the results, consent and data in the
patient profile
4. Release the results or give results access to
patient
5. Communicate the results with other
healthcare professionals that the patient
chooses.
55Dr. Dalia A. Hamdy (FS 19/20AY)
 Pharmacists are encouraged to communicate
with local physicians and introduce them to
report samples
 Physicians are expected to act positively if
they are aware and familiar with the shape
or the results.
 Pharmacists should encourage the patients to
contact their physicians if the results
warrants any change in therapy
56Dr. Dalia A. Hamdy (FS 19/20AY)
 A pharmacist must prepare the dr. to the
referral . Surprises are not recommended!
57Dr. Dalia A. Hamdy (FS 19/20AY)
58Dr. Dalia A. Hamdy (FS 19/20AY)

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A Hands on Pharmacogenomics! An Introduction

  • 1. Pharm 503 4th November 2019 Dalia A. Hamdy BSc.(Pharm), MSc., PhD, RPh., MBA, MRSC Founder and Manager of AbEx Health Services LTD. Clinical Assistant Professor, FoPPS, University of Alberta dhamdi@ualberta.ca 2-142K Katz
  • 2. i. Getting introduced to the basics of pharmacogenomics and its effect on drug metabolism/pharmacokinetics (PK) and/or pharmacodynamics (PK-PD). ii. Apply Pharmacogenomics in precision medicine iii. Having a Hands-on experience on the online resources used to help you find dosing guidelines (CPIC & PharmGKb) iv. Integrating pharmacogenenomics into your clinical assessment and decision in resolving drug therapy problems and optimizing pharmacotherapy outcomes Dr. Dalia A. Hamdy (FS 19/20AY) 2
  • 3. 1. Langman L, Dasgupta A. Pharmacogenomics in Clinical Therapeutics.; Wiley-Blackwell 2012. 2. CPIC Guidelines for Simvastatin and SLCO1B1 https://www.pharmgkb.org/chemical/PA451363/guidelineAnnotation/ PA166105005 3. Roden D. Case Studies in personalized medicine. Vanderbilt University. Online course through coursera. https://www.coursera.org/lecture/personalizedmed/variability-in-drug- therapy-spi4r 4. CPIC Guidelines for codeine and CYP2D6 https://www.pharmgkb.org/guidelineAnnotation/PA166104996 5. CPIC Guidelines for clopidogrel and CYP2C19 https://www.pharmgkb.org/guidelineAnnotation/PA166104948 6. CPIC Guidelines for voriconazole and CYP2C19 https://www.pharmgkb.org/chemical/PA10233/guidelineAnnotation/P A166161537 7. Klein D. et al. PharmGKB summary: tamoxifen pathway, pharmacokinetics. Pharmacogenet Genomics. 2013; 23(11): 643–647. 3Dr. Dalia A. Hamdy (FS 19/20AY)
  • 4. 1. SLCO1B1 is a (transporter/enzyme/receptor) that is found in the hepatocytes also known as (OATP1B1/OAT1B1/OCT1B1). The following Allelle(s) (*1a/*5/*14/*2) has normal function whereas (*1a/*5/*14/*2) has decreased function and (*1a/*5/*14/*2) has increased function. 2. A patient shows up in your pharmacy with a genotype of (*1a/*1a) what would be the recommended dose? Can we give 80 mg qd for this patient? Why? What is your reference? 3. A patient carrying a genotype of (*1a/*5) came across your pharmacy and his cholesterol levels were not adjusted using the 20 mg /day dose of statin? What would be your recommendation? 4Dr. Dalia A. Hamdy (FS 19/20AY)
  • 5. 5Dr. Dalia A. Hamdy (FS 19/20AY)
  • 6. 6Dr. Dalia A. Hamdy (FS 19/20AY)
  • 7. 7Dr. Dalia A. Hamdy (FS 19/20AY)
  • 8. 8Dr. Dalia A. Hamdy (FS 19/20AY)
  • 9. 9Dr. Dalia A. Hamdy (FS 19/20AY)
  • 10. “is the tailoring of medical treatment to the individual characteristics of each patient” The Age of Personalized Medicine “The science of individualized prevention and therapy” National Institute of Health 10Dr. Dalia A. Hamdy (FS 19/20AY)
  • 11. 11 One Size fits all medicine Vs. Personalized medicine Dr. Dalia A. Hamdy (FS 19/20AY)
  • 12. 12Dr. Dalia A. Hamdy (FS 19/20AY)
  • 13. Pharmacogenetics: The study of the effect of variations in DNA sequence (genetic differences) on drug response in terms of both the metabolism/clearance (PK) and action (PD) of the drug delivered 13Dr. Dalia A. Hamdy (FS 19/20AY)
  • 14. 14Dr. Dalia A. Hamdy (FS 19/20AY)
  • 15. 15Dr. Dalia A. Hamdy (FS 19/20AY) 1. What is DNA? DNA (deoxyribonucleic acid),  the cell’s hereditary material.  DNA is a polymer of nucleotides (sugar, phosphate and one of four nitrogenous bases (A,T,G,C)
  • 16. Human genome consists of about 3.2 billion base pair (bp) Every person has two copies of each gene, one inherited from each parent (6.4 billion bp) DNA molecule is packaged into thread-like structures called chromosomes. 23 pairs of Chromosomes  Sex chromosome XX or XY  22 pairs autosomes 16Dr. Dalia A. Hamdy (FS 19/20AY)
  • 17. 2. What is the gene function? DNA • 99-98% Non-coding : its job is to actually regulate the process whereby genes are translated into proteins. • 1-2% coding : acts like the blueprint that encodes proteins (enzymes, structural elements, signaling molecules) 17Dr. Dalia A. Hamdy (FS 19/20AY)
  • 18. 3. Types of polymorphism -SNPs (Single-Nucleotide Polymorphisms) –Indels(Insertions & Deletions) –VNTR (Variable Number Tandem Repeats) –CNV (Copy Number Variants) –Haplotypes (combination of alleles or to a set of single nucleotide polymorphisms (SNPs) found on the same chromosome 18Dr. Dalia A. Hamdy (FS 19/20AY)
  • 19.  Gene mutations  Inherited from a parent  Acquired during a person’s lifetime  Mutations range in size from  single base-pair mutation that occurs at a specific site in the DNA sequence (SNV)  to a large segment of a chromosome (CNV) 19 SNP = SNV which occur in at least 1-2% of the population Dr. Dalia A. Hamdy (FS 19/20AY)
  • 20. 3. Types of genetic variants SNP can be in the coding or non-coding regions of the DNA resulting in different proteins that could be functional or non functional 20Dr. Dalia A. Hamdy (FS 19/20AY)
  • 21. 21Dr. Dalia A. Hamdy (FS 19/20AY)
  • 22. • Polymorphism in enzymes, receptors and transporters proteins can affect the PK and PD of several medications • In fact, 50–75% of medications are substrates of the cytochrome P450 (CYP) 3A4 enzyme, 2C9, and/or 2D6 metabolizing enzymes • 50% of CPIC drugs guidelines involves 2C19, and/or 2D6 22Dr. Dalia A. Hamdy (FS 19/20AY)
  • 23. 23Dr. Dalia A. Hamdy (FS 19/20AY)
  • 24. 24Dr. Dalia A. Hamdy (FS 19/20AY)
  • 25. Genes Alleles CYP1A2 *1C, *1C, *1E,*1F, *1J, *1K, *1L, *1V, *1W, *6, *7, *8, *15 CYP2B6 *2, *4, *5, *6, *7, *8, *9, *13, *16, *18, *22, *34 CYP2C19 *2, *3, *4, *4B, *6, *8, *10, *17 CYP2C9 *2, *3, *4, *5, *6, *8, *9, *11, *12, *18, *27 CYP2D6 *2, *2A, *3, *4, *5, *6, *7, *9, *10, *14, *14A, *17, *29, *4N, *4M, *5, *6, *6C, *7, *8, *9, *10, *11, *12, *13, *14A, *14B, *15, *17, *18, *19, *29, *31, *34, *35, *36, *39,*41, *42, *63, *64, *68, *69, *70, *91, *109 CYP3A4 *1B, *3, *6, *11, *12, *16, *17, *18, *19, *22 CYP3A5 *2, *3A, *3B, *6, *7 COMT VAL158MET DPYD *2A, *4, *5, *6, *9A, *13, rs7376798A DRD2 PROMOTER VARIANT -241A>G F2 20210G>A F5 ARG534GLN (LEIDEN, 1691G>A) GRIK4 NON-CODING (INTRONIC) T>C VARIANT HTR2A INTRON 2, T>C VARIANT HTR2C PROMOTER VARIANT -759C>T IFNL3 rs1297860 C/T IL28B (IFNL4) NON-CODING (INTRONIC) C>T VARIANT NUDT15 ARG139CYS OPRM1 ASN40ASP, A118G SLC6A4 C,-1810A>G; -1791_-1749DEL43 SLCO1B1 *1B, *5, *9, *15, *31 TPMT *2, *3A, *3B, *3C, *4, *8 UGT1A1 *6, *27, *38, *60, *80 VKORC1 c.-1639G>T, A and G variants 25 Commercially available pharmacogenomic testing available in the Canadian market Dr. Dalia A. Hamdy (FS 19/20AY)
  • 26. 1. A patient appears with a T4 prescription in your pharmacy. While discussing with him the use and checking his history you realize that he has been on T3 and the pain is not manageable and the dr. moved him to T4. In few days, he appears again with a higher dose of codeine and still his pain is not in control. -would you recommend a pharmacogenetic testing for this patient? Why? -If his PGX results came like that CYP2D6 *4/*7, CYP2C19*1/*17, CYP2C9*1/*1, VKORC1 AA What would you recommend and why? 2. What if the patient carried CYP2D6 *4/*9? 3. Knowing the mechanism of action of codeine, What other information could be missing? 26Dr. Dalia A. Hamdy (FS 19/20AY)
  • 27. 1. CYP 2D6 27Dr. Dalia A. Hamdy (FS 19/20AY)
  • 28. 1. CYP 2D6 This had been determined using genotyping and phenotyping. In phenotyping, a CYP2D6 specific probe drug such as dextromethorphan is administered the relative ratio between the concentration of probe drug (dextromethorphan: DM) and its CYP2D6 specific metabolite (dextorphan:DX)is obtained. DM:DX ratios poor metabolizers. DM:DX ratios extensive metabolizers 28Dr. Dalia A. Hamdy (FS 19/20AY)
  • 29. 1. CYP 2D6 29Dr. Dalia A. Hamdy (FS 19/20AY)
  • 30. 1. CYP 2D6 30Dr. Dalia A. Hamdy (FS 19/20AY)
  • 31. 1. CYP 2D6 What is the effect of 2D6 on codeine? Codeine • Opiate analgesic • Prodrug of morphine - is found naturally but at low concentrations so usually synthesized from morphine 31Dr. Dalia A. Hamdy (FS 19/20AY)
  • 32. 1. CYP 2D6 32Dr. Dalia A. Hamdy (FS 19/20AY)
  • 33. 33 1. Codeine is bioactivated to morphine, a strong opioid agonist, by the hepatic cytochrome P450 2D6 2. The efficacy and safety of codeine are governed by CYP2D6 activity. 3. Polymorphisms are a major cause of CYP2D6 variability. Dr. Dalia A. Hamdy (FS 19/20AY)
  • 34. Dr. Dalia A. Hamdy (SS18/19AY) 34
  • 35. 35 Similarly What about CYP2D6 and Tamoxifen? Tamoxifen: • a selective estrogen receptor modulator • Used for the treatment and prevention of estrogen receptor (ER)-positive breast cancer • The drug is extensively metabolized by CYP2D6 and other enzymes. Dr. Dalia A. Hamdy (FS 19/20AY)
  • 36. 36Dr. Dalia A. Hamdy (FS 19/20AY)
  • 37. 37 Similarly What about CYP2D6 and Tamoxifen? • 4-hydroxytamoxifen and endoxifen, are more potent and considered the primary active forms of the drug. Dr. Dalia A. Hamdy (FS 19/20AY)
  • 38. 38 Phenotype Genotype Therapeutic recommendation for tamoxifen Ultrarapid metabolizer More than two copies of functional alleles None Intermediate metabolizer One active allele and one inactive allele, or two decreased activity alleles, or one decreased activity allele and one inactive allele Increased risk for relapse of breast cancer. Avoid concomitant use of CYP2D6 inhibitors. Consider aromatase inhibitor for postmenopausal women Poor metabolizer Two inactive alleles Increased risk for relapse of breast cancer. Consider aromatase inhibitor for postmenopausal women Dr. Dalia A. Hamdy (FS 19/20AY)
  • 39. 39Dr. Dalia A. Hamdy (FS 19/20AY)
  • 40. 40Dr. Dalia A. Hamdy (FS 19/20AY)
  • 41. 41Dr. Dalia A. Hamdy (FS 19/20AY)
  • 42. 42Dr. Dalia A. Hamdy (FS 19/20AY)
  • 43. 43Dr. Dalia A. Hamdy (FS 19/20AY)
  • 44. 44Dr. Dalia A. Hamdy (FS 19/20AY)
  • 45. 45 PCI:Percutaneous coronary intervention ACS: Acute coronary syndromeDr. Dalia A. Hamdy (FS 19/20AY)
  • 46. 46Dr. Dalia A. Hamdy (FS 19/20AY)
  • 47. 47Dr. Dalia A. Hamdy (FS 19/20AY)
  • 48. 48 1. What is expected to happen when I have a. PM or IM CYP2C19? b. UM or RM CYP2C19? 2. If we know that voriconazole is used for ttt of invasive fungal infections in cancer patients. Also that trough concentrations <2 mcg/ml is associated with worse clinical outcomes? What are the CPIC guidelines for a pt. with CYP2C19 *1/*17 or *2/*3? Dr. Dalia A. Hamdy (FS 19/20AY)
  • 49. 49Dr. Dalia A. Hamdy (FS 19/20AY)
  • 50. 50Dr. Dalia A. Hamdy (FS 19/20AY)
  • 51. 51Dr. Dalia A. Hamdy (FS 19/20AY)
  • 52. 52 Using the CPIC guidelines how would you consider carbamazepine therapy in the following pts. 1. A patient was using CBZ for 4 months and stopped for problems with insurance coverage and hospitalization periods. The dr. wants to restart him again on CBZ. The dr. phones you and asks that he heard about an available pharmacogenomic test that is needed for this pt.? Would you strongly recommend doing the test ? For what gene? Why/why not? 2. The patient did the test and those were the results CYP2D6 *4/*7, CYP2C19*1/*17, CYP2C9*1/*1, VKORC1 AA, HLA-B*15:02 negative What would you suggest the dr. to do? Dr. Dalia A. Hamdy (FS 19/20AY)
  • 53. 53 Using the CPIC guidelines how would you consider carbamazepine therapy in the following pts. 3. A naïve pt. patient wants to start CBZ therapy and his genetic testing shows HLA- A*31:01 genotype What would you suggest the dr. to do? Dr. Dalia A. Hamdy (FS 19/20AY)
  • 54. 54 Discussion point Dr. Dalia A. Hamdy (FS 19/20AY)
  • 55. Pharmacists are expected to 1. Be the point of testing for the patients 2. Receive the patients reports and interpret them in a meeting in lay language 3. Keep the results, consent and data in the patient profile 4. Release the results or give results access to patient 5. Communicate the results with other healthcare professionals that the patient chooses. 55Dr. Dalia A. Hamdy (FS 19/20AY)
  • 56.  Pharmacists are encouraged to communicate with local physicians and introduce them to report samples  Physicians are expected to act positively if they are aware and familiar with the shape or the results.  Pharmacists should encourage the patients to contact their physicians if the results warrants any change in therapy 56Dr. Dalia A. Hamdy (FS 19/20AY)
  • 57.  A pharmacist must prepare the dr. to the referral . Surprises are not recommended! 57Dr. Dalia A. Hamdy (FS 19/20AY)
  • 58. 58Dr. Dalia A. Hamdy (FS 19/20AY)

Editor's Notes

  1. Transporter, oatp1B1 1a 5 14 Normal, check the recommendation, either through guidelines or through the imbedded results on website
  2. The approach relies on scientific breakthroughs in our understanding of how a person’s unique molecular and genetic profile makes them susceptible to certain diseases. This same research is increasing our ability to predict which medical treatments will be safe and effective for each patient, and which ones will not be.
  3. The approach relies on scientific breakthroughs in our understanding of how a person’s unique molecular and genetic profile makes them susceptible to certain diseases. This same research is increasing our ability to predict which medical treatments will be safe and effective for each patient, and which ones will not be.
  4. Cnv copy number variations
  5. Single nucleotide variants CNV copy number variants Alleles are forms of the same gene with small differences in their sequence of DNA bases. These small differences contribute to each person’s unique physical features
  6. Missence: polymorphism changes amino acid composition (missense) Nonesense:induces premature stop codons (nonsense), thereby affecting protein function. although they may affect gene expression (promoter SNPs) or RNA splicing
  7. CPIC:The Clinical Pharmacogenetics Implementation Consortium
  8. Discuss the cl and dose and auc and relationships and general expectations
  9. 3. The u receptor mutations
  10. Uridine 5'-diphospho-glucuronosyltransferase (UDP-glucuronosyltransferase, UGT) is a cytosolic glycosyltransferase (EC 2.4.1.17) that catalyzes the transfer of the glucuronic acid component of UDP-glucuronic acid to a small hydrophobic molecule. This is a glucuronidation reaction.