AI Article Synopsis

  • Rasagiline is a drug used to treat Parkinson's disease by inhibiting a specific enzyme (monoamine oxidase type B) and has neuroprotective effects.
  • The study assessed the influence of different genetic variations on how the body processes rasagiline in 118 healthy volunteers, finding that certain gene variations affected the drug's absorption and distribution.
  • The findings indicate that genetic differences in drug transporters are more significant in affecting rasagiline's pharmacokinetics than variations in metabolizing enzymes, with minimal adverse reactions reported.

Article Abstract

Rasagiline is a selective and irreversible inhibitor of monoamine oxidase type B with neuroprotective effect, indicated for the management of Parkinson's disease. The aim of this work was to evaluate the impact of seven alleles and of 120 additional variants located in other CYP enzymes (e.g., ), UGT enzymes (e.g., ) or other enzymes (e.g., ), and transporters (e.g., ) on the pharmacokinetic variability and safety of rasagiline. A total of 118 healthy volunteers enrolled in four bioequivalence clinical trials consented to participate in this pharmacogenetic study. alleles were not associated with the pharmacokinetic variability of rasagiline. Patients with rs1045642 G/A+A/A genotypes presented higher area under the curve adjusted by dose per weight (AUC/DW) than those with the G/G genotype ( = 0.012) and lower volume of distribution (V/F) and clearance (Cl/F) ( = 0.001 and = 0.012, respectively). Subjects with the rs2273697 A/A genotype presented lower t (i.e., the time to reach the maximum concentration, C) compared to those with G/G+G/A genotypes ( = 0.001). Volunteers with the *1/*5 genotype exhibited lower C/DW and higher t ( = 0.003 and = 0.018, respectively) than subjects with the *1/*1 diplotype. Only one adverse drug reaction was reported: headache. Our results suggest the genetic polymorphism of drug transporters, rather than metabolizing enzymes, conditions the pharmacokinetics of rasagiline.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9610285PMC
http://dx.doi.org/10.3390/pharmaceutics14102001DOI Listing

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