Which of the following statements represents the most clinically significant aspect of drug metabolism?

Most common enzyme involved is CYP 3A4/5

Glucuronidation is a phase II reaction

Reduction is a phase I reaction

Cytochrome P450 is involved in phase I reactions

Which of the following cytochromes is involved in monooxygenase mediated detoxification of drugs?

NADPH-cytochrome P450 reductase

In X-linked recessive (XLR) diseases, a modified inheritance pattern called 'pseudodominance' occurs when?

One parent is an unaffected heterozygote and the other is an affected homozygote.

One parent is an affected homozygote and the other is an unaffected homozygote.

One parent is normal and the other is an unaffected heterozygote.

Pharmacogenomics for FMGE: High-Yield Internal Medicine Lessons

Pharmacogenomics Basics - Gene-Drug Dance

Definition: Study of how an individual’s genetic makeup influences their response to drugs. Aims for personalized medicine: maximizing efficacy, minimizing toxicity.
Core Principle: Genetic variations (e.g., Single Nucleotide Polymorphisms - SNPs, Copy Number Variations - CNVs) in genes coding for:
- Drug-metabolizing enzymes (e.g., Cytochrome P450 family like CYP2D6, CYP2C19)
- Drug transporters (e.g., SLCO1B1)
- Drug targets (e.g., VKORC1 for warfarin)
Impacts: Primarily Pharmacokinetics (PK - what the body does to the drug, especially metabolism) and Pharmacodynamics (PD - what the drug does to the body).
Resulting Phenotypes (examples for metabolizing enzymes):
- Poor Metabolizers (PM): ↓ enzyme activity → ↑ drug levels, ↑ risk of toxicity.
- Ultrarapid Metabolizers (UM): ↑ enzyme activity → ↓ drug levels, risk of therapeutic failure.
- Extensive Metabolizers (EM): Normal enzyme activity.
- Intermediate Metabolizers (IM): Between PM and EM.

⭐ Over 200 drugs now have pharmacogenomic information in their FDA-approved labeling, highlighting its growing clinical importance.

Key Pharmacogenes - Enzyme & Transporter Tales

Key Pharmacogenes and Drug Response

Gene (Product)	Key Drug(s)	Variant Implication	Note/Mnemonic
CYP2D6 (Enzyme)	Codeine, Tamoxifen	PMs: ↓ efficacy/ADRs (Codeine: ↓ analgesia). UMs: ↑ toxicity.	📌 2D6: Diverse Drugs, 6 phenotypes
CYP2C9 (Enzyme)	Warfarin, Phenytoin	↓ activity (2,3): ↑ Warfarin levels, bleeding risk. Dose ↓.
CYP2C19 (Enzyme)	Clopidogrel, PPIs	PMs (2,3): ↓ Clopidogrel activation → risk CV events. UMs (*17): ↑ bleeding.	📌 Clopi-2C19: Cardiac Concern
TPMT (Enzyme)	Azathioprine, 6-MP	↓ activity: ↑ TGNs → myelosuppression. Test before.
UGT1A1 (Enzyme)	Irinotecan	*28 (Gilbert's): ↓ SN-38 glucuronidation → ↑ toxicity (diarrhea, neutropenia).
SLCO1B1 (OATP1B1)	Statins (Simvastatin)	c.521T>C: ↓ statin uptake → ↑ plasma levels → myopathy risk.	📌 SLCO: Statin Level Control
VKORC1 (Enzyme target)	Warfarin	Variants: affect warfarin sensitivity. Dose adjustment.	Warfarin's target
DPYD (Enzyme)	5-FU, Capecitabine	Deficiency: ↓ catabolism → severe toxicity.
HLA-B*57:01 (MHC)	Abacavir	AHS risk. Mandatory screening.	⭐ > HLA-B*57:01 screening for abacavir prevents severe hypersensitivity.
HLA-B*15:02 (MHC)	Carbamazepine	SJS/TEN risk (Asians). Test before.

Clinical Applications - Prescribing Pointers

Pharmacogenomics guides personalized drug therapy, optimizing efficacy and minimizing adverse drug reactions (ADRs). Key clinical examples:

Warfarin: CYP2C9, VKORC1 variants.
- Altered metabolism/sensitivity.
- Requires dose adjustments to prevent bleeding/clotting.
Clopidogrel: CYP2C19 loss-of-function alleles.
- Prodrug; poor metabolizers (PMs) have ↓ activation, ↑ risk of stent thrombosis.
- Consider alternatives (prasugrel, ticagrelor) in PMs.
Abacavir (HIV): HLA-B*57:01 allele.
- Strong association with abacavir hypersensitivity (AHR).
- Screening mandatory; contraindicated if positive.
Azathioprine/6-MP: TPMT, NUDT15 variants.
- ↓ enzyme activity → ↑ drug levels.
- High risk of severe myelosuppression. Dose reduction needed.
Carbamazepine: HLA-B*15:02 (Asians), HLA-A*31:01 (Europeans).
- Risk of SJS/TEN. Screening recommended in specific populations.
Codeine: CYP2D6 polymorphisms.
- Ultra-rapid metabolizers (UMs): risk of toxicity.
- Poor metabolizers (PMs): ↓ analgesia.
Irinotecan: UGT1A1*28 (Gilbert's).
- ↓ activity → ↑ SN-38. Risk of neutropenia, diarrhea. Dose reduction.

⭐ HLA-B*57:01 testing before abacavir initiation has dramatically reduced the incidence of hypersensitivity reactions, making it a cornerstone of HIV therapy safety.

Pharmacogenomic variants impact on drug prescribing

High‑Yield Points - ⚡ Biggest Takeaways

CYP2D6 polymorphisms impact codeine metabolism; poor metabolizers (PMs) have ↓ efficacy, ultra-rapid metabolizers (UMs) risk toxicity.

CYP2C19 variants affect clopidogrel activation; PMs have ↑ risk of stent thrombosis.

TPMT/NUDT15 deficiency causes severe toxicity with thiopurines (azathioprine, 6-MP).

HLA-B*5701 screening is crucial before abacavir to prevent hypersensitivity.

Warfarin dosing is guided by CYP2C9 and VKORC1 genotypes.

SLCO1B1 variants increase risk of statin-induced myopathy.

G6PD deficiency predisposes to drug-induced hemolytic anemia (e.g., primaquine).

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