Table of Contents

Reviews

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  • Pavlina T. Ivanova,
  • Stephen B. Milne,
  • Jeffrey S. Forrester,
  • and H. Alex Brown

  LIPID Arrays: New Tools in the Understanding of Membrane Dynamics and Lipid Signaling

  Mol Interv April 2004 4:86-96; doi:10.1124/mi.4.2.6
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  Once regarded as little more than a tiny bag whose sole purpose was to retain the really interesting constituents of the cell, the plasma membrane is now appreciated for its vital elegance. Cell surface receptors in particular have become a staple of biomedical research, and the turnover of membrane phospholipid is a fundamental concept in signal-transducing mechanisms. Still, the dynamic complexity of lipid signaling has gone largely unexplored, primarily due to difficulties in identifying the multiple lipid species that fall under each of a slew of rubrics, such as “phosphoinositide,” “phosphatidylcholine,” and “diacylglycerol.” Today, advancing technologies in mass spectrometry and computational analysis promise to deliver detailed snapshots of the full complement of lipid species over the course of cellular responses to physiological cues.

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  • Natalie J. Serkova,
  • Uwe Christians,
  • and Leslie Z. Benet

  Biochemical Mechanisms of Cyclosporine Neurotoxicity

  Mol Interv April 2004 4:97-107; doi:10.1124/mi.4.2.7
  • Abstract
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  Of the several immunosuppressive drugs used to facilitate organ transplantation, the undecapeptide cyclosporine serves as a cornerstone in the prevention of graft rejection. A high percentage of treated patients, however, suffer from serious neurotoxic side effects. Paradoxically, cyclosporine ameliorates brain injury induced by cerebral ischemia–reperfusion in vivo, and this neuroprotective function has magnified interest in elucidating the biochemical mechanisms of cyclosporine action in the central nervous system. Magnetic resonance spectroscopy (MRS) is being increasingly used to quantify metabolic consequences of drug neurotoxicity and has revealed that cyclosporine evokes morphological changes in the brain.

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  • Dennis L. Murphy,
  • Alicja Lerner,
  • Gary Rudnick,
  • and Klaus-Peter Lesch

  Serotonin Transporter: Gene, Genetic Disorders, and Pharmacogenetics

  Mol Interv April 2004 4:109-123; doi:10.1124/mi.4.2.8
  • Abstract
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  The serotonin transporter (SERT) modulates the concentration of serotonin in extracellular fluids. Given this essential role, genetic variability in SERT is of considerable interest in elucidating disorders of serotoninergic activity. Genetic disturbances within the chromosome 17q region where SERT is located have been mapped and may be associated with a variety of disorders, including autism, attention deficit-hyperactivity disorder, bipolar disorder, and Tourette’s syndrome. Studies of knockout mice, moreover, suggest SERT as a determinant of additional clinical conditions, ranging from irritable bowel syndrome to obesity. The association of certain polymorphisms with poorer therapeutic responses to SERT antagonists, including more frequent serious side effects, also has important implications for the treatment of emotional disorders.