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Published Online: 1 February 2011

Thought, Feeling, and Action in Real Time—Monitoring of Drug Use in Schizophrenia

In this issue, Swendsen and colleagues (1) report that substance use, mood states, and psychotic symptoms in schizophrenia patients can be measured in real time. The findings in this article offer a new strategy for investigating cause-and-effect relationships between environmental influences and psychopathology.
Early support for a link between substance use and psychosis onset came from a 15-year follow-up of Swedish conscripts, which found that heavy cannabis use was related to an increased risk for schizophrenia (2). Subsequent cohort studies have similarly reported that the use of cannabis and other “street drugs” increases the risk of psychosis onset (3, 4). In turn, several groups have explored the question of whether substances are used as an attempt to self-medicate psychotic symptoms or to alleviate dysphoria, but the results of such studies have been mixed (5, 6).
An inherent limitation to this literature is that it is usually necessary to rely on retrospective self-report and clinical assessments for data collection. Moreover, in a population of patients with known impairments in episodic memory (7), the reliability of retrospective clinical data may be particularly limited. Thus, the use by Swendsen and colleagues of computerized ambulatory monitoring techniques to assess temporal relationships between subjective experiences and events offers a novel and powerful new strategy to study behaviors and their motivation in real time. Similar studies have been conducted by this group to study alcohol use (8) and other aspects of the syndrome of schizophrenia (9).
Swendsen and colleagues (1) used computerized ambulatory monitoring to record alcohol or drug use and psychotic symptoms and mood states in 145 schizophrenia patients. The schizophrenia patients were trained to use a personal digital assistant (PDA) to complete 15-minute electronic interviews, and the PDAs were programmed to prompt the participant four times each day (between 9:00 a.m. and 9:00 p.m.) for 1 week. The study findings revealed that the use of cannabis increased the risk of experiencing psychotic symptoms, while decreasing perceived negativity. In contrast, the use of alcohol was not temporally associated with the risk of experiencing psychotic symptoms or negative mood states. The use of “other” substances (e.g., cocaine, opiates, amphetamines) also increased the risk of experiencing psychotic symptoms or anxiety. Finally, Swendsen and colleagues completed the circle of cause and effect by showing that the presence of psychotic symptoms was related to later use of alcohol or other drugs, while anxiety, sadness, and perceiving events as negative were related to the later use of alcohol, cannabis, and other illicit drugs. Drilling deeper into each of these temporal relationships revealed specific relationships between different psychopathological states and substances.
The authors appropriately controlled for the status of predicted outcomes as they existed at the moment the predictor variable was assessed. They also controlled for other confounds, such as time of day, medication use, and polysubstance use. As noted by the authors, the conclusions that can be drawn from this study are somewhat limited because of the lack of data on the frequency and duration of substance use. Moreover, the findings may also be less applicable to schizophrenia patients with more severe negative symptoms, as such patients may have been more likely to decline participation and more likely to refuse completion once participation began. Last, given that substance use can peak during the evening hours, it would be interesting in future studies to examine the use of substances and negative outcomes at time points later than the 9:00 p.m. limit used in the current study.
Despite these minor limitations, this study has substantial clinical and methodological importance. First, the ability to measure hourly fluctuations in substance use, psychosis, and negative mood states can help advance our knowledge of the temporal relationships among events, behavior, and internal experience. The results of this study provide support for the growing consensus that cannabis and perhaps other drugs can trigger psychotic symptoms. In turn, the results of this study also provide support for prior claims of self-medication for dysphoria (10), since cannabis and alcohol use followed the experience of psychotic symptoms and negative mood states. In sum, it appears that the “arrow” of cause and effect is circular and points back onto itself. Second, the authors have further validated the use of computerized ambulatory monitoring techniques for collecting real-time data in a challenging clinical population. This technique could potentially be extended to estimate the quantity, frequency, and duration of a variety of behaviors and internal psychological states in many other groups of patients. Moreover, it could be utilized in the context of treatment to better understand adherence to, and the effects of, psychotropic medications on an hourly or daily basis.
Nearly 50% of schizophrenia patients have a lifetime diagnosis of a comorbid substance use disorder (11). Thus, new interventions are badly needed to reduce the motivation of schizophrenia patients to use drugs and to reduce the effects of such drugs on internal experience and behavior. The work presented in this issue by Swendsen and colleagues (1) demonstrates that the use of a novel technique, computerized ambulatory monitoring, is feasible and can be used to unravel relationships between substance use, experience, and psychopathology. Beyond the use of such technology in clinical research, it is tantalizing to think that computerized ambulatory monitoring might find a role in the clinic one day. What clinician has not struggled to understand the event or thought that preceded an action in a patient? Real-time ambulatory monitoring offers a new strategy for reaching out to our patients and for our patients to reveal their experiences to us.

Footnotes

Editorial accepted for publication November 2010
Dr. Csernansky reports receiving honoraria for serving on data monitoring committees for Eli Lilly and Sanofi-Aventis. Dr. Freedman has reviewed this editorial and found no evidence of influence from these relationships.

References

1.
Swendsen J, Ben-Zeev D, Granholm E: Real-time electronic ambulatory monitoring of substance use and symptom expression in schizophre-nia. Am J Psychiatry 2011; 168:202–209
2.
Andreasson S, Allebeck P, Engstrom A, Rydberg U: Cannabis and schizophrenia: a longitudinal study of Swedish conscripts. Lancet 1987; 2:1483–1486
3.
Henquet C, van Os J, Kuepper R, Delespaul P, Smits M, Campo JA, Myin-Germys I: Psychosis reactivity to cannabis use in daily life: an ex-perience sampling study. Br J Psychiatry 2010; 196:447–453
4.
Smith MJ, Thirthalli J, Abdallah AB, Murray RM, Cottler LB: Prevalence of psychotic symptoms in substance users: a comparison across sub-stances. Compr Psychiatry 2009; 50:245–250
5.
Brunette MF, Mueser KT, Xie H, Drake RE: Relationships between symptoms of schizophrenia and substance abuse. J Nerv Ment Dis 1997; 185:13–20
6.
Talamo A, Centorrino F, Tondo L, Dimitri A, Hennen J, Baldessarini RJ: Comorbid substance-use in schizophrenia: relation to positive and negative symptoms. Schizophr Res 2006; 86:251–255
7.
Leavitt VM, Goldberg TE: Episodic memory in schizophrenia. Neuropsychol Rev 2009; 19:312–323
8.
Johnson EI, Barrault M, Nadeau L, Swendsen J: Feasibility and validity of computerized ambulatory monitoring in drug-dependent women. Drug Alcohol Depend 2009; 99:322–326
9.
Granholm E, Loh C, Swendsen J: Feasibility and validity of computerized ecological momentary assessment in schizophrenia. Schizophr Bull 2008; 34:507–514
10.
Gregg L, Barrowclough C, Haddock G: Reasons for increased substance use in psychosis. Clin Psychol Rev 2007; 27:494–510
11.
Buckley PF: Substance abuse in schizophrenia: a review. J Clin Psychiatry 1998; 59(suppl 3):26–30

Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 120 - 122
PubMed: 21297046

History

Accepted: November 2010
Published online: 1 February 2011
Published in print: February 2011

Authors

Details

John G. Csernansky, M.D.
Matthew J. Smith, Ph.D., M.P.E., M.S.W.

Notes

Address correspondence and reprint requests to Dr. Csernansky, Department of Psychiatry and Behavioral Sciences, Northwestern University Feinberg School of Medicine, Suite 7-100, 446 East Ontario St., Chicago, IL 60611; [email protected] (e-mail).

Funding Information

Dr. Smith reports no financial relationships wit commercial interests.

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