The 2009 Schizophrenia PORT Psychopharmacological Treatment Recommendations and Summary Statements

The Schizophrenia Patient Outcomes Research Team (PORT) psychopharmacological treatment recommendations provide a comprehensive summary of current evidence-based pharmacological treatment practices. There have been 2 previous sets of pharmacological treatment recommendations.^1,2 These recommendations have served to guide the development of algorithms^3,4 and guidelines⁵ for the treatment of schizophrenia.

Since the last update of the PORT psychopharmacological treatment recommendations,² there have been over 600 studies published on the pharmacological treatment of schizophrenia. These have included a series of publications from 3 large pragmatic studies: the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE),⁶ the Cost Utility of the Latest Antipsychotic Drugs in Schizophrenia Study (CUtLASS),⁷ and the European First-Episode Schizophrenia Trial (EUFEST).⁸ The CATIE and CUtLASS studies represent the 2 largest, non-industry sponsored comparisons of first-generation antipsychotic (FGA) medications and second-generation antipsychotic (SGA) medications in people with multi-episode schizophrenia, whereas EUFEST compared haloperidol to multiple SGAs in people with first-episode schizophrenia. In addition, there have been a series of new studies that have examined antipsychotic monotherapy and adjunctive strategies for the treatment of a number of symptom and behavioral outcomes, including cognitive impairments, negative symptoms, and co-occurring medical and substance misuse disorders. The number of publications in these areas warrants the evaluation of the pharmacological treatment of these outcomes. Finally, although not a pharmacological intervention, there have been a number of studies that have evaluated the potential efficacy of repetitive transcranial magnetic stimulation (rTMS) for the treatment of refractory auditory hallucinations.

In the current PORT update, we evaluated published studies to determine whether the current PORT psychopharmacological treatment recommendations required revision and whether there was sufficient evidence to warrant new treatment recommendations for prespecified outcomes of interest.

The Schizophrenia PORT Psychopharmacology Evidence Review Group (ERG) was comprised of University of Maryland Baltimore faculty with expertise in the pharmacological treatment of schizophrenia. The Psychopharmacology ERG was charged with 2 tasks: (1) to review new evidence related to the extant PORT psychopharmacological treatment recommendations and (2) in consultation with the Psychopharmacology Advisory Board, to identify new outcomes or interventions to review for the purpose of determining whether a treatment recommendation was warranted for the outcome or intervention. These outcomes and interventions included but were not limited to antidepressants, antipsychotic polypharmacy, cognition, electroconvulsive therapy (ECT), negative symptoms, rTMS, smoking cessation, and quality of life.

On a quarterly basis, the Psychopharmacology ERG conducted electronic MEDLINE literature searches, using as search terms “schizophrenia” and the names of individual antidepressants, antiepileptics, antipsychotics, benzodiazepines, and lithium; schizophrenia; and clinical trial as search terms. Other search terms included specific topic areas, such as treatment of cognition, extrapyramidal side effects, first-episode schizophrenia, negative symptoms, prolactin-related side effects, quality of life, tardive dyskinesia (TD), and weight gain. All searches were limited to English language, clinical trial, and schizophrenia and to medications with U.S. Food and Drug Administration approval.

The time period for the literature search was January 2002 through March 2008. In addition, if appropriate for the evaluation of an intervention or outcome, we included articles published prior to January 2002, if the area had not previously undergone a PORT review. We did not re-review articles published prior to January 2002, if they had been reviewed in one of the previous PORT treatment recommendation publications. If a relevant article was published after March 2008 and would significantly alter the PORT evaluation of the evidence, then the article was included in the reviewed evidence base.

Each Psychopharmacology ERG member was assigned one or more antipsychotic medication and designated topic areas to review, with 2 ERG members assigned to each antipsychotic medication to ensure that all relevant articles were identified and included in the review. At the quarterly Psychopharmacology ERG meetings, the members would present the article abstracts from their literature search. If the study was a randomized controlled trial (RCT), and at least 50% of the participants had a schizophrenia spectrum disorder diagnosis, that is, schizophrenia, schizoaffective disorder, or schizophreniform disorder, then the article was selected for further review. The majority of studies were double-blind RCTs, with the following major exceptions: one of the CATIE phase 2 studies,⁹ the CUtLASS study,⁷ and EUFEST.⁸ In the CATIE phase 2E study, the clozapine arm was open labeled⁹; in the CUtLASS study, participants were randomly assigned to open-label antipsychotic treatment, with clinical raters blind to treatment assignment⁷; and in the EUFEST study, participants were randomly assigned to open-label antipsychotic treatment and the majority of clinical ratings were not blinded to treatment assignment.⁸ In addition, we would also allow case reports or case series, if the outcome was a rare event, eg, neuroleptic malignant syndrome (NMS).

In the case of the extant PORT pharmacological treatment recommendations, the selected articles were reviewed for their potential to importantly modify these recommendations. In the case of new interventions or outcomes, there were 2 possible review results. First, the reviewed evidence could meet criteria for sufficient evidence to merit a treatment recommendation (see Kreyenbuhl et al,¹⁰ this issue, for a description of these criteria). Alternatively, the evidence could be judged to be insufficient to merit a treatment recommendation, in which case a summary statement was written that described the intervention, the indication for the intervention, and provided a summary of the evidence and the important gaps in knowledge that precluded treatment recommendation status. The draft treatment recommendations and summary statements were then reviewed by the external advisory board (see Kreyenbuhl et al,¹⁰ this issue, for a description of this process) and their comments were incorporated into revisions, which were re-reviewed by the external advisory board, and then final versions were produced.

There are 16 treatment recommendations. The treatment recommendations are grouped either by intervention or outcome. The presentation of each treatment recommendation follows the same format: the title of the treatment recommendation, the full recommendation, the expert rating of the treatment recommendation, and the evidence summary for the recommendation.

There were 13 interventions or outcomes for which there was insufficient evidence to warrant a treatment recommendation. A summary of the intervention or outcome, the evidence to date and future areas of investigation are presented for each of these areas. The summaries are grouped either by intervention or outcome. A more detailed presentation of the available evidence for the intervention is presented in the online supplemental materials. The absence of a treatment recommendation should not be construed as a proscription against the particular practice. Rather, the interventions may be potentially beneficial, but at the time of the PORT review, the evidence did not reach the level to warrant the designation of an evidence-based practice.

The Schizophrenia PORT Psychopharmacology ERG reviewed over 400 studies on pharmacological and other somatic treatments of schizophrenia, which resulted in 16 treatment recommendations: we updated 11 previous treatment recommendations; we identified 5 additional treatment areas for which the evidence was sufficiently strong to support a treatment recommendation; and we eliminated 3 previous recommendations. We reviewed for the first time pharmacological treatments for a number of health conditions that disproportionately affect individuals with schizophrenia, including cigarette smoking, drug addiction, and weight gain resulting from antipsychotic treatment. These reviews led to a new PORT recommendation for a combined psycho-pharmacological and psychosocial approach to smoking cessation, a significant unmet treatment need and major public health concern in this population. The other new recommendations include the choice of antipsychotic agent for the treatment of people with first-episode schizophrenia, monitoring clozapine levels, antipsychotic treatment of acute agitation, and rTMS for the short-term treatment of refractory auditory hallucinations. There were 13 reviewed areas for which the scientific evidence was currently insufficient to support a treatment recommendation.

Three previous 2004 Schizophrenia PORT treatment recommendations were dropped: (1) clozapine for NMS, tardive dystonia, and TD; (2) monitoring antipsychotic blood levels; and (3) the use of antidepressants to treat depression in people with schizophrenia. In the place of the treatment recommendation for clozapine and NMS, tardive dystonia, and TD, 2 summary statements have been written, which review the epidemiology of TD and NMS and the current status of the treatment or management of these antipsychotic side effects. The decision to drop the antidepressant treatment recommendation reflected the surprising lack of evidence for this practice. Since the last PORT update, few rigorous studies on the effectiveness of newer antidepressants (eg, selective serotonin reuptake inhibitors [SSRIs]) for depressive symptoms in schizophrenia, particularly among people treated with SGAs, have been published. The previous PORT recommendation for antidepressant treatment was largely based on studies of older tricyclic antidepressants in people treated with FGAs, both medication classes that have fallen out of widespread use in clinical practice. Moreover, on reevaluation, these previous studies were judged to provide less compelling evidence for this practice than originally thought.^1,2 Therefore, in light of the lack of new evidence with SGAs and selective serotonin reuptake inhibitors (SSRIs) and the lack of compelling evidence for tricyclic antidepressants, the current level of evidence for antidepressant treatment in schizophrenia was determined to be insufficient to support a treatment recommendation, and the previous recommendation was rescinded.

There are a number of review outcomes that are worthy of specific mention. First, since its inception almost 15 years ago, the Schizophrenia PORT has been consistent in not recommending the preferential use of SGAs vs FGAs in the acute or maintenance treatment of people with treatment-responsive, multi-episode schizophrenia. Although initially an unpopular stance that was inconsistent with prevailing prescribing patterns and public opinion, the relative efficacy/effectiveness of FGAs and SGAs was not a controversial issue in the current Schizophrenia PORT update. In large part, this was due to the recent completion of 2 large pragmatic clinical trials: the CATIE and CUtLASS studies.^6,7,48 These publicly funded investigations, which featured head-to-head comparisons of the relative effectiveness of multiple SGAs and representative FGAs, found very few effectiveness differences across these agents. The results of CATIE and CUtLASS, thus, provided strong support for the long-standing Schizophrenia PORT position that antipsychotic medication selection should not be limited to a particular agent or class of drug but rather tailored to the individual characteristics and preferences of each person with schizophrenia.

Second, the CATIE and CUtLASS studies, along with recent investigations in individuals experiencing their first episode of schizophrenia, have added to the growing evidence base regarding the differential side effect profiles across antipsychotic agents. Of particular concern has been the mounting evidence that certain SGAs are associated with significant weight gain and metabolic abnormalities that may lead to long-term adverse health consequences in an already at-risk population. The relative clinical equivalence of FGAs and SGAs has, thus, shifted the focus of antipsychotic selection to the side effects of these agents, and because of the propensity of olanzapine, in particular, to induce metabolic side effects, this PORT update includes a new recommendation for withholding the use of olanzapine as a first-line choice for antipsychotic treatment in first-episode schizophrenia. This new recommendation, however, should not be construed as an absolute proscription against the use of olanzapine in the treatment of schizophrenia. Rather, the PORT recommends that other antipsychotic medications be considered before a trial of olanzapine in newly diagnosed individuals for whom maximizing the acceptability of the initial treatment experience and minimizing both short- and long-term treatment risks is especially crucial.

Third, the CATIE and CUtLASS studies also made major contributions to the already strong body of research, demonstrating that clozapine is the most effective antipsychotic medication available for individuals who continue to experience persistent and clinically significant positive symptoms after adequate trials of other antipsychotic agents. The PORT continues its strong endorsement of the use of clozapine for this indication as well as for the treatment of hostility and violence and suicidal behaviors, domains for which effective treatments are not otherwise available. Although the gap between science and service has been typically more evident for psychosocial treatments than for psychopharmacological treatments,¹³⁶ clozapine represents an important exception. Although the precise reasons for the persistent underutilization of clozapine in clinical practice are not entirely understood, concerns about required monitoring for agranulocytosis and the development of other troublesome adverse effects are likely contributory.¹³⁷ Efforts to more fully understand the reluctance on the part of both prescribers and eligible patients to consider a trial of this widely available, evidence-based treatment are clearly needed.

Fourth, in marked contrast to the strong evidence supporting the effectiveness of clozapine and other antipsychotic medications for the core symptoms of schizophrenia, there is a relative paucity of information on the effectiveness of adjunctive pharmacological agents for the treatment of persistent positive symptoms or other symptom domains, including depressive symptoms, anxiety, cognitive impairments, and persistent negative symptoms. The lack of evidence-based treatments for these indications is notable given the extent to which adjunctive antidepressants, mood stabilizers, anti-anxiety agents, antipsychotics, and other medications are used in typical clinical practice.¹³⁸ The discrepancy between the relatively widespread use of adjunctive psychotropic medications and the lack of evidence to support these practices reflects, in part, the quandary that clinicians face when confronted with the person who has failed to adequately respond to antipsychotic monotherapy or has additional symptoms for which antipsychotic agents are known to be ineffective. Under these circumstances, the use of non–evidence-based practices requires that the clinician be especially conscientious in documenting whether the patient is responding to the intervention and be prepared to discontinue the treatment if a desired response is not achieved.² The development of effective treatments for the ancillary symptoms of schizophrenia is of critical importance because these domains are often major barriers to recovery.

Finally, our most recent review of the literature revealed a number of areas of psychopharmacological treatment for schizophrenia for which the determination of whether the scientific evidence was sufficiently strong to support a recommendation was not straightforward. A major area of discussion among the PORT Expert Panel involved the nature of the evidence for the effectiveness of switching antipsychotic medications for the treatment of antipsychotic-related weight gain. The process of switching antipsychotic agents due to side effects, especially in individuals who are experiencing a significant reduction in symptoms or improvement in functional outcomes, should consider the potential benefits from side effect reduction vs the risks of symptom exacerbation. In clinical practice, if the risk/benefit ratio is appropriate, physicians in consultation with their patients should allow for trials of antipsychotic switching with the goal of the treatment of weight loss or any other medication side effect. The practice of switching an antipsychotic medication has been a very effective strategy for the treatment of a number of medication side effects including EPS, prolactin elevation, and sedation. However, to develop a PORT treatment recommendation in this area, we required a minimal level of evidence that the majority of individuals would experience significant weight loss without clinical deterioration. While the studies we reviewed suggest that switching antipsychotic medications does lead to weight loss, especially among individuals treated with olanzapine, there is only one un-replicated RCT that has directly examined this issue, and some participants in that study who switched from olanzapine to aripiprazole experienced worsening of their clinical status. The ongoing Comparison of Antipsychotics for Metabolic Problems) study⁴⁹ should help clarify the usefulness of switching antipsychotic medications for the treatment of weight gain in schizophrenia and may lead to a future treatment recommendation in this important area. Other evidence-based approaches to weight loss for people with schizophrenia are available because the evidence supporting psychosocial interventions is currently sufficient to support a PORT treatment recommendation (see Dixon et al,¹³⁵ this issue).

The other area for which there was notable discussion among the Expert Panel concerned the decision to recommend specific dosage ranges for the acute and maintenance treatment of schizophrenia and the treatment of first-episode schizophrenia. In particular, there was concern over the quality of the data used to select the lower and upper dose ranges and the potential adverse policy impact that might result from the stipulation of a dose range. The recommended dose ranges represent those doses for which there is documented efficacy from RCTs and for which the observed side effects do not compromise the beneficial effects of the particular agent. The lower end of the dose range has been fairly well established for most drugs through industry-sponsored, double-blind, fixed-dose studies. The problem lies with the upper range for a number of the SGAs, for which adequate upper dose range data are not available for aripiprazole, olanzapine, quetiapine, and ziprasidone. In addition, as discussed in the previous Schizophrenia PORT update,² there is the problem of central tendency, in which the results of clinical trials provide information on the mean effect in the population studied. There are multiple reasons why an individual may not respond to a drug prescribed within the recommended dose range, including increased sensitivity to side effects or rapid metabolism of the drug. Therefore, the PORT recommended dose ranges should serve only as guidelines for the clinician. They are not proscriptions against the use of doses outside the recommended range but a reminder that there should be some rationale provided for the use of a nonrecommended dosage.

In summary, over the past 5 years, there have been marked gains in our knowledge of evidence-based pharmacological treatments for schizophrenia. In order to ensure that all people with schizophrenia receive the highest quality pharmacological treatment, providers of mental health services should strive to ensure that each of these evidence-based practices is readily available for those patients for whom the treatments are indicated. However, despite these recent advances, there remain a number of important gaps in our knowledge of how to address treatment needs that lie outside the core symptom domains of schizophrenia. These gaps are important barriers to the ultimate goal of improving the individualized treatment of the person with schizophrenia and optimizing their opportunity for recovery from the illness.

Supplementary material is available at http://schizophreniabulletin.oxfordjournals.org.

National Institute of Mental Health (R13 MH080593 to J.K.); the Department of Veterans Affairs (Mental Health Enhancement Grant to J.K.).

The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institute of Mental Health, the National Institutes of Health, or the Department of Veterans Affairs. The authors would like to acknowledge the following members of the Schizophrenia PORT Psychopharmacology Advisory Board: Susan M. Essock, PhD; Donald C. Goff, MD; Richard S. E. Keefe, PhD; Stephen R. Marder, MD; John W. Newcomer, MD; Diana O. Perkins, MD, MPH; T. Scott Stroup, MD, MPH. The authors would also like to acknowledge Jeanette Robinson for retrieving copies of articles and organizing and managing the database of studies reviewed for this update of the Schizophrenia PORT Psychopharmacological Treatment Recommendations. R.W.B.: Data and Safety Monitoring Board member: Cephalon and Pfizer; Consultant: Abbott, Glaxo-Smith-Kline, Natixis Bleichroeder, Sanofi-Aventis, Schering-Plough; Advisory Board: Astra-Zeneca, Merck, Pfizer, Roche, Solvay Pharmaceuticals, Inc., Wyeth, Grant Support: Janssen Pharmaceutica; D.L.K.: Advisory Board: Bristol Myers Squibb, Janssen Pharmaceutica, and Solvay. Julie Kreyenbuhl, Jason M. Noel, Douglas L. Boggs, Bernard A. Fischer, Seth Himelhoch, Beverly Fang, Eunice Peterson, Patrick R. Aquino, and William Keller have no competing interests or financial support to disclose.