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To the Editor: We are highly appreciative of the excellent contributions provided by the authors of this letter, most of whom are members of the DSM-5 Substance-Related Disorders Work Group. We also welcome the opportunity to focus additional attention on the differences between previous DSM field trials and those conducted for DSM-5. Contrary to the initial statement in the Hasin et al. letter, test-retest reliability was a major focus of the DSM-5 field trials, but not of the DSM-IV field trial—the latter being more concerned about changes in prevalence that would occur if the same patients were examined using DSM-III, DSM-III-R, and ICD-10 criteria in contrast to the minimally changed DSM-IV criteria (1). The reliability of DSM-IV criteria for substance use disorders noted by Hasin et al. was derived from multiple studies unrelated to the DSM-IV field trial, employing highly trained interviewers using structured research interviews. These studies were often epidemiological with a special interest in substance use disorders (2)—not conducted in routine clinical settings where DSM is most widely used without the use of structured diagnostic interviews.
In research settings, it is well known that it is possible to maximize reliability, regardless of the validity of a diagnosis, by using selected populations, structured interviews, and highly trained interviewers. Robert Spitzer noted this in a 1997 review of the progression of diagnostic systems to that point in time: “Many studies show that researchers using structured interviews and assessing targeted populations (e.g., patients attending an anxiety disorder clinic) can achieve high reliability. However, the reliability of diagnosis in actual clinical practice by clinicians who have varying commitment to actually using the DSM criteria is unknown, but is probably low” (3, p. 13).
The use of clinicians (or nonclinicians) with special training and required structured interviews would indeed explain the discrepancy of kappas. That would mean that, as a measure of how reliable the diagnosis would be in routine practice, the DSM-IV kappas are overestimates. In turn, as a measure of how reliable the DSM-5 diagnosis could be under the ideal conditions that usually do not pertain in practice, DSM-5 kappas are underestimates (4). Again we get back to the reliability of diagnosis under ideal conditions versus the reliability of diagnosis under usual conditions. Which one is of interest: that which affects patient care or that which could be obtained under ideal conditions for research purposes?
This is the same argument as used for efficacy versus effectiveness trials (5). Does one want to know how a treatment works under ideal conditions with patients with no other comorbid conditions, a rare occurrence in actual practice, or how a treatment works if clinicians use it with their patients under usual conditions? This question may be answered quite differently when asked of clinicians and patients or investigators trying to develop new treatments. The distinction is crucial since treatments that work well under ideal conditions may perform differently when used in clinical settings.
With that in mind, the decision was made early in the development of DSM-5 to focus on improving the lot of psychiatric patients and to leave the optimization of diagnosis in research settings to the researchers in those settings. It was recognized that DSM-5 reliabilities would be lower than reported DSM-IV reliabilities done under ideal conditions, but would be comparable to reliabilities of many medical diagnoses (6). We thought it was timely to invest resources in determining how our diagnostic criteria would function in usual settings, which could also advance our understanding of the validity of DSM-5 diagnoses.

References

1.
Cottler LB, Schuckit MA, Helzer JE, Crowley T, Woody G, Nathan P, Hughes J: The DSM-IV field trial for substance use disorders: major results. Drug Alcohol Depend 1995; 38:59–69, discussion 71–83
2.
Hasin D, Hatzenbuehler ML, Keyes K, Ogburn E: Substance use disorders: Diagnostic and Statistical Manual of Mental Disorders, fourth edition (DSM-IV) and International Classification of Diseases, tenth edition (ICD-10). Addiction 2006; 101(suppl 1):59–75
3.
Spitzer RL: From Feighner to RDC, DSM-III, DSM-III-R, DSM-IV and ICD-10: how the Feighner Criteria transformed world psychiatry, in The Feighner Criteria: Their Role in Psychiatric Progress: A 25th Anniversary Review. Edited by, Winokur G. Secaucus, NJ, Churchill Communications North America, 1997
4.
Regier DA, Narrow WE, Clarke DE, Kraemer HC, Kuramoto SJ, Kuhl EA, Kupfer DJ: DSM-5 field trials in the United States and Canada, part II: test-retest reliability of selected categorical diagnoses. Am J Psychiatry 2013; 170:59–70
5.
March JS, Silva SG, Compton S, Shapiro M, Califf R, Krishnan R: The case for practical clinical trials in psychiatry. Am J Psychiatry 2005; 162:836–846
6.
Kraemer HC, Kupfer DJ, Narrow WE, Clarke DE, Regier DA: Moving toward DSM-5: the field trials. Am J Psychiatry 2010; 167:1158–1160

Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 443 - 444
PubMed: 23545796

History

Accepted: February 2013
Published online: 1 April 2013
Published in print: April 2013

Authors

Details

Darrel A. Regier, M.D., M.P.H.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
Helena C. Kraemer, Ph.D.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
William Narrow, M.D., M.P.H.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
Diana E. Clarke, Ph.D., M.Sc.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
S. Janet Kuramoto, Ph.D., M.H.S.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
Emily A. Kuhl, Ph.D.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.
David J. Kupfer, M.D.
From the American Psychiatric Association, Division of Research and American Psychiatric Institute for Research and Education, Arlington, Va.; the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore; the Stanford University School of Medicine, Palo Alto, Calif.; and the University of Pittsburgh Medical Center, Pittsburgh.

Competing Interests

The authors’ disclosures accompany the original article.

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