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Non-MAO A binding of clorgyline in white matter in human brain
Authors:J. S. Fowler,J. Logan,Y.-S. Ding,D. Franceschi,G.&#  J. Wang,N. D. Volkow,N. Pappas,D. Schlyer,S. J. Gatley,D. Alexoff,C. Felder,A. Biegon&dagger  , W. Zhu&Dagger  
Affiliation:Chemistry Department, Brookhaven National Laboratory, Upton, New York 11973, USA. fowler@bnl.gov
Abstract:Clorgyline is an irreversible inhibitor of monoamine oxidase (MAO A) which has been labeled with carbon-11 (C-11) and used to measure human brain MAO A with positron emission tomography (PET). In this study we compared [11C]clorgyline and deuterium-substituted [11C]clorgyline ([11C]clorgyline-D2) to better understand the molecular link between [11C]clorgyline binding and MAO A. In PET studies of five normal healthy volunteers scanned with [11C]clorgyline and [11C]clorgyline-D2 2 h apart, deuterium substitution generally produced the expected reductions in the brain uptake of [11C]clorgyline. However, the reduction was not uniform with the C-11 binding in white matter being significantly less sensitive to deuterium substitution than other brain regions. The percentages of the total binding attributable to MAO A is largest for the thalamus and smallest for the white matter and this is clearly seen in PET images with [11C]clorgyline-D2. Thus deuterium-substituted [11C]clorgyline selectively reduces the MAO A binding component of clorgyline in the human brain revealing non-MAO A binding which is most apparent in the white matter. The characterization of the non-MAO A binding component of this widely used MAO A inhibitor merits further investigation.
Keywords:clorgyline    human brain    monoamine oxidase A    white matter
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