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Pharmacogenetics • Definitions – Pharmacogenetics: single gene differences among population groups and the effects on pharmacodynamics. – Pharmacegenomics: genome-wide variations in DNA sequences responsible for pharmacodynamic differences. – In practice, these two terms are used interchangeably. Pharmacogenetics • Human genome comprised of approximately 30,000 genes from a total of 3 billion base pairs. • Different base-pair combinations result in different proteins produced. • Single base mutation can alter a produced protein (enzyme) significantly. • Result is that different population groups have somewhat different proteins and enzymes. Pharmacogenetics • Some population groups may metabolize some compounds very rapidly, whereas another group may metabolize the same compound slowly. This can lead to overdose or underdose situations. • Understanding important pharmacogenetic differences among populations allows better drug and/or dosage choices for a particular need. Pharmacogenetics • Examples: – Multidrug Resistance Gene can cause differences in absorption of some drugs (digoxin) by altering carrier proteins or barrier compounds in the GI tract. – 5-hydroxytryptamine transporter polymorphisms can affect the neuronal reuptake of serotonin, an important neurotransmitter. – Plasma cholinesterase, which readily breaks down succinylcholine, tetracaine, mivacurium, etc., is seen in some individuals to have reduced activity, which can cause increased duration of these compounds. Pharmacogenetics • Examples: – Many different CYP genes identified. Results in different metabolic rates of some drugs by individuals. • CYP2D6 shows widest known differences, since it is responsible for approximately 25% of all drug metabolism, including analgesics, neuroleptics, antiarrhythmics, amide-type LA’s, beta blockers, TCA’s, and antiemetics. • CYP2C9 responsible for metabolism of warfarin, phenytoin, NSAIDS • NAT responsible for metabolism of Isoniazid (INH), sulfonamides, procainamide • NAT polymorphisms show fast (Asian) and slow (European) types. Pharmacogenetics • Ethnicity – While obvious phenotypic differences exist among some ethnic groups, it is impossible to tell a persons complete genetic background ‘on-sight’. – Due to recent (last 100 years) world-wide population mixing, different genes are mixing in the overall population, making it almost impossible to be sure of any ethnically-carried genetic differences. Pharmacogenetics • Sex – Several differences in drug metabolism rates have been identified between males and females: • Females clear drugs oxidized by CYP3A4 40% faster than males. • Many conjugation (Phase II) metabolic reactions occur at a faster rate in males than females. • Females also demonstrated to have lower pain tolerance, greater opioid sensitivity, and higher risk of Halothane toxicity than males. • Females awaken 50% faster from propofol/alfentanil/nitrous oxide anesthesia than men, and may require greater doses to reach proper anesthesia levels. Pharmacogenetics • Practical Considerations – With so many defined differences, why has pharmacogenetics not become more important in practice of anesthesia? • Requires genetic testing, which concerns people. • Costs and time of screening. – Many of the 3% of untoward outcomes of anesthesia are believed to be attributed to pharmacogenetic differences in the population, and could be alleviated. – Changes are occuring, and will slowly be implemented.