
Am J Psychiatry 165:46A, August 2008
doi: 10.1176/appi.ajp.2008.165.8.A46
© 2008 American Psychiatric Association
In This Issue
Progress in Treating Schizophrenia
Improvement in patient functioning has become a yardstick for measuring new treatments for schizophrenia. Mohamed et al. (p. 978) found that patients psychiatric symptoms and cognition both contribute to functioning, as reflected in quality of life ratings and employment. In addition, in the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE), functional changes were related to changes in symptoms and cognition over 18 months of treatment. Two studies of new antipsychotic treatments illustrate this dual outcomes assessment. Shekhar et al. (CME, p. 1033) evaluated xanomeline, a selective agonist of acetylcholine muscarinic receptors. Compared to 10 patients randomly assigned to placebo, the 10 assigned to xanomeline had greater improvement in global outcomes, positive and negative schizophrenia symptoms, verbal learning, and short-term memory. Freedman et al. (p. 1040) compared two doses of a partial 7 nicotinic cholinergic agonist, DMXB-A, with placebo in a crossover trial. The higher DMXB-A dose was associated with greater improvement in negative symptoms, especially alogia and anhedonia, than placebo. Improvements in attention and working memory occurred with DMXB-A during the first arm of the trial. Dr. Jeffrey Lieberman et al. comments in an editorial on p. 931.
Anatomical Changes in Schizophrenia
Two comparisons of brain structure in first-episode and chronic schizophrenia suggest declines in both gray and white matter. The meta-analysis by Ellison-Wright et al. (p. 1015) of voxel-based data from 27 MRI studies indicates a progressive decrease of gray matter volume in the frontal, insular, and temporal cortices. Progression of pathology from the hippocampus to the amygdala was not found. Using diffusion tensor imaging, Friedman et al. (p. 1024) examined white matter structure in 80 patients. Those with chronic schizophrenia had modestly lower values than matched healthy subjects, and the differences reached statistical significance in the right forceps minor and left inferior longitudinal fasciculus. First-episode patients did not differ from healthy subjects, but progression was suggested by similarities between first-episode and chronically ill patients in abnormalities in three regions. An editorial by Drs. John Csernansky and Will Cronenwett on p. 937 focuses on these findings.
What Makes Aripiprazole Different?
Most second-generation antipsychotic medications preferentially bind to receptors outside the striatum, but Gründer et al. (p. 988) report that aripiprazole attaches to dopamine receptors throughout the brain. Positron emission tomography also showed that aripiprazole occupied over 80% of dopamine D2 and D3 receptors in patients with schizophrenia. Further, these receptors remained saturated for several days after the last dose. Occupancy values correlated with blood levels of aripiprazole but not with daily dose. Dr. Donald Goff examines these characteristics in an editorial on p. 940.
Schizophrenia Frontal Brain Dysfunction
Differing methods revealed similar findings about brain functioning in schizophrenia. Ferrarelli et al. (p. 996) measured electrical activity in the frontal cortex by using direct magnetic stimulation. The evoked gamma-frequency oscillations were markedly less in patients with schizophrenia than in healthy subjects. Both amplitude and synchronization were affected, particularly in the fronto-central region. Activation was also more localized, suggesting impaired connectivity between regions. Yoon et al. (CME, p. 1006) examined the dorsolateral prefrontal cortex during a task requiring cognitive control of contingent behavior. Functional magnetic resonance imaging revealed less activity in the patients with schizophrenia than in matched healthy subjects. The patients also had less connectivity between this region and other task-related brain regions. The changes in prefrontal connectivity were strongly associated with symptoms of disorganization, impaired cognition, and lower social and occupational functioning. An editorial by Drs. Daniel Mathalon and Judith Ford on p. 944 reviews implications of these results.
Related Articles:
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Cholinergic Agonists as Novel Treatments for Schizophrenia: The Promise of Rational Drug Development for Psychiatry
- Jeffrey A. Lieberman, Jonathan A. Javitch, and Holly Moore
Am J Psychiatry 2008 165: 931-936.
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Neural Networks in Schizophrenia
- John G. Csernansky and Will J. Cronenwett
Am J Psychiatry 2008 165: 937-939.
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New Insights Into Clinical Response in Schizophrenia: From Dopamine D2 Receptor Occupancy to Patients Quality of Life
- Donald C. Goff
Am J Psychiatry 2008 165: 940-943.
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Divergent Approaches Converge on Frontal Lobe Dysfunction in Schizophrenia
- Daniel H. Mathalon and Judith M. Ford
Am J Psychiatry 2008 165: 944-948.
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Selective Muscarinic Receptor Agonist Xanomeline as a Novel Treatment Approach for Schizophrenia
- Anantha Shekhar, William Z. Potter, Jeffrey Lightfoot, John Lienemann, Sanjay Dubé, Craig Mallinckrodt, Frank P. Bymaster, David L. McKinzie, and Christian C. Felder
Am J Psychiatry 2008 165: 1033-1039.
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Association of Dorsolateral Prefrontal Cortex Dysfunction With Disrupted Coordinated Brain Activity in Schizophrenia: Relationship With Impaired Cognition, Behavioral Disorganization, and Global Function
- Jong H. Yoon, Michael J. Minzenberg, Stefan Ursu, Ryan Walters, Carter Wendelken, J. Daniel Ragland, and Cameron S. Carter
Am J Psychiatry 2008 165: 1006-1014.
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Initial Phase 2 Trial of a Nicotinic Agonist in Schizophrenia
- Robert Freedman, Ann Olincy, Robert W. Buchanan, Josette G. Harris, James M. Gold, Lynn Johnson, Diana Allensworth, Alejandrina Guzman-Bonilla, Bettye Clement, M. Patricia Ball, Jay Kutnick, Vicki Pender, Laura F. Martin, Karen E. Stevens, Brandie D. Wagner, Gary O. Zerbe, Ferenc Soti, and William R. Kem
Am J Psychiatry 2008 165: 1040-1047.
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The Anatomy of First-Episode and Chronic Schizophrenia: An Anatomical Likelihood Estimation Meta-Analysis
- Ian Ellison-Wright, David C. Glahn, Angela R. Laird, Sarah M. Thelen, and Ed Bullmore
Am J Psychiatry 2008 165: 1015-1023.
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Brain and Plasma Pharmacokinetics of Aripiprazole in Patients With Schizophrenia: An [18F]Fallypride PET Study
- Gerhard Gründer, Christine Fellows, Hildegard Janouschek, Tanja Veselinovic, Christian Boy, Anno Bröcheler, Katrin M. Kirschbaum, Sandra Hellmann, Katja M. Spreckelmeyer, Christoph Hiemke, Frank Rösch, Wolfgang M. Schaefer, and Ingo Vernaleken
Am J Psychiatry 2008 165: 988-995.
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Diffusion Tensor Imaging Findings in First-Episode and Chronic Schizophrenia Patients
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Am J Psychiatry 2008 165: 1024-1032.
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Relationship of Cognition and Psychopathology to Functional Impairment in Schizophrenia
- Somaia Mohamed, Robert Rosenheck, Marvin Swartz, Scott Stroup, Jeffrey A. Lieberman, and Richard S.E. Keefe
Am J Psychiatry 2008 165: 978-987.
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Reduced Evoked Gamma Oscillations in the Frontal Cortex in Schizophrenia Patients: A TMS/EEG Study
- Fabio Ferrarelli, Marcello Massimini, Michael J. Peterson, Brady A. Riedner, Mariana Lazar, Michael J. Murphy, Reto Huber, Mario Rosanova, Andrew L. Alexander, Ned Kalin, and Giulio Tononi
Am J Psychiatry 2008 165: 996-1005.
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