Table of Contents

Viewpoints

• • Bianca Rocca and
  • Giovanna Petrucci

  Personalized Medicine, Pharmacogenetics, and Clopidogrel: Unraveling Variability of Response

  Mol Interv February 2010 10:12-19; doi:10.1124/mi.10.1.4
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  In 1997, clopidogrel was approved in the US for the prevention of cardiovascular diseases and received EU approval one year later. The large heterogeneity of the individual pharmacodynamic response of patients to this drug at the recommended doses was evident quite soon after marketing. Nevertheless, the mechanism(s) underlying this variability have been more clearly characterized in the past five years. The in vivo generation of the active metabolite from the pro-drug clopidogrel is the final result of a complex balance between bio-activating and bio-inactivating enzymatic reactions. The complex pharmacokinetics—not pharmacodynamics—of clopidogrel has been recognized as a major source of individual variability in drug response, as assessed by diverse assays of platelet inhibition. Pharmacogenetics and drug interactions modulate the enzymatic efficiency of the two-step bioactivating processes, which are mediated by different subfamilies of the cytochromes P (CYP) 450. Genetic variants of some CYP450s affect the generation of active metabolite, platelet (pharmacodynamic) response, and clinical outcomes of clopidogrel-treated patients. These findings have rapidly brought clopidogrel into the "personalized medicine" realm.

• • KyeongEun Lee and
  • Kathryn S. Jones

  The Path Well Traveled: Using Mammalian Retroviruses to Guide Research on XMRV

  Mol Interv February 2010 10:20-24; doi:10.1124/mi.10.1.5
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  The xenotropic murine leukemia virus-related virus (XMRV) was first detected several years ago in prostate cancer tissue. A recent report links this virus to a different type of human disease, chronic fatigue syndrome (CFS), and demonstrates that infectious virus can be isolated from the blood of infected individuals. CFS has previously been linked to the presence of other viruses, including human herpes virus-6 and Epstein-Barr virus, but a causal relationship was never proven; thus, the new finding of an association to XMRV has stirred some controversy. Although XMRV, like HIV, is a retrovirus, XMRV is most closely related to viruses found in the genomes of certain mice. The large body of knowledge generated during decades of studying both human and non-human retroviruses provides important clues about the biology of XMRV and approaches for the development of therapeutic regimens. If there is something that both believers and skeptics can agree on, it is that an ongoing investigation is needed to clarify some of the current mysteries involving the biology of XMRV replication and its threat to human health.