^{Symptom remission is the desired goal of treatment for depression, given its implications for better daily functioning and better longer-term prognosis. Since no treatment is a panacea, several sequential treatment steps are often needed to obtain remission with a tolerated treatment. If a trial does not result in remission, it is an unsuccessful trial, whether due to lack of efficacy or intolerable side effects, as long as the treatment is vigorously dosed to tolerance and provided for a sufficient duration to achieve remission. The number of treatment steps needed to achieve an adequate benefit is typically used to gauge the degree of treatment resistance, usually with a focus on acute outcomes without reference to longer-term outcomes.}

^{After two treatment steps, it appears that over 50% of patients will achieve remission if they stay in treatment (i.e., 36.8% step 1 plus 30.6% of the remaining 63.2% of patients). Thereafter, the chances of subsequent remission are much lower. The theoretical cumulative remission rate after four acute treatment steps was 67%.}

Acute and longer-term outcomes in depressed outpatients requiring one or several treatment steps: a STAR*D report.
by Rush AJ, Trivedi MH, Wisniewski SR, Nierenberg AA, Stewart JW, Warden D, Niederehe G, Thase ME, Lavori PW, Lebowitz BD, McGrath PJ, Rosenbaum JF, Sackeim HA, Kupfer DJ, Luther J, Fava M.
Am J Psychiatry. 2006 Nov;163(11):1905-17.

Abstract

^{OBJECTIVE: This report describes the participants and compares the acute and longer-term treatment outcomes associated with each of four successive steps in the Sequenced Treatment Alternatives to Relieve Depression (STAR*D) trial.}

^{METHOD: A broadly representative adult outpatient sample with nonpsychotic major depressive disorder received one (N=3,671) to four (N=123) successive acute treatment steps. Those not achieving remission with or unable to tolerate a treatment step were encouraged to move to the next step. Those with an acceptable benefit, preferably symptom remission, from any particular step could enter a 12-month naturalistic follow-up phase. A score of <or=5 on the Quick Inventory of Depressive Symptomatology-Self-Report (QIDS-SR(16)) (equivalent to <or=7 on the 17-item Hamilton Rating Scale for Depression [HRSD(17)]) defined remission; a QIDS-SR(16) total score of >or=11 (HRSD(17)>or=14) defined relapse.}

^{RESULTS: The QIDS-SR(16) remission rates were 36.8%, 30.6%, 13.7%, and 13.0% for the first, second, third, and fourth acute treatment steps, respectively. The overall cumulative remission rate was 67%. Overall, those who required more treatment steps had higher relapse rates during the naturalistic follow-up phase. In addition, lower relapse rates were found among participants who were in remission at follow-up entry than for those who were not after the first three treatment steps.}

^{CONCLUSIONS: When more treatment steps are required, lower acute remission rates (especially in the third and fourth treatment steps) and higher relapse rates during the follow-up phase are to be expected. Studies to identify the best multistep treatment sequences for individual patients and the development of more broadly effective treatments are needed.}

If this is your first time with the STAR*D trial, it’s unlikely that this flow-chart is very clarifying, so I’ve simplified the chart on the right for our perusal, removing the details. In this trial "Exit" means drop-out. After each level of treatment, some number of subjects elect to stop. That group is designated as "Follow-Up" but only a portion of those are in remission [the numbers in gray and green come from Table 3 in the article]. So the 67% is a hypothetical wish in virtual reality, not what the study actually demonstrated. And what of the drop-outs [38% of the subjects who entered some form of treatment dropped out]? In the paper, the authors say:

^{The cumulative remission rate can be estimated by assuming that 100 patients begin citalopram treatment. Overall, 36.8 will achieve remission in step 1, leaving 63 to proceed to the next step. In step 2, 30.6% (N=19) will remit (.306×63 = 19). In the third step, 13.7% or N=6 will remit (.137 x [100–37-19]). In the fourth step, 13.0% or N=5 will remit. The theoretical cumulative remission rate is 67% (37+19+6+5). Note that this estimate assumes no dropouts, and it assumes that those who exited the study would have had the same remission rates as those who stayed in the protocol.}

^{1. The STAR*D investigators reported a "cumulative" remission rate of 67% in the abstract of an article, when in fact this was simply a "theoretical" rate.}
^{2. They reported remission rates based on the QIDS-SR scale, even though the pre-specified primary outcome scale was the HRSD, and this switch inflated the remission numbers.}
^{3. They included remission numbers for patients who weren’t depressed enough at baseline to meet study criteria, and thus weren’t eligible for analysis.}
^{4. They reported that 33.3% to 50% of remitted patients relapsed during the 12-year followup, which suggested – when combined with the inflated 67% remitted rate – that perhaps 40% of all patients who entered the trial had recovered and stayed well, when in fact only 3% of the entering patients had a "sustained remission" [and stayed in the trial].}

What I think about STAR*D

I’m not an anti-psychiatrist. I’m a psychiatrist and have prescribed many [but not all] of the drugs mentioned in this study. But I didn’t review the study for this last week or so because I believed what it said or to learn anything about treating depressed people. Nobody who uses these medications and actually sees patients could possibly believe those conclusions. I read it to collect my thoughts about the psychiatrists who wrote it and the government agency that funded it. One of my conclusions was easy – these authors are anti-psychiatrists. Who needs a psychiatrist to collect a list of symptoms, conclude that the person is depressed from that list, then plug the depressed person into an algorithmic protocol like the one they describe? I’m not even sure you would need a doctor or trained mental health professional. An overqualified Walmart greeter I met recently could do that quite well.

As an Internist, I saw lots of depressed people. I didn’t follow the path suggested here even back then. I learned to ask those patients about their lives, their relationships, their experiences. But I didn’t have to ask very much. Just asking anything at all got them started talking and I learned a lot about why they were depressed, but I didn’t know what to do with what I learned – and I wanted to. So I came back and did a Psychiatry Residency to find out what to do, fortunately in the pre-STAR*D days. Had the notions in this study been the curriculum, I would have happily returned to Internal Medicine. Instead, I learned that depression was a human emotion we can all experience. I learned that sometimes, it can be a disease, like in Manic Depressive Illness, or Post-Partum Depression, or when you take certain medicines, etc. But most of the time, it’s a starting place to signal that it’s time to start untying some of those knots that experience has a way of tying in our lives and minds. And that’s what I did for thirty years, learn to help people with the untying. It’s what I wanted to learn back in the Internist days and it was worth the trip.

I gave [and give] the medications. For a few, they’re a godsend. For others, they help to a varying degree. But I never conceived this – "Symptom remission is the desired goal of treatment for depression, given its implications for better daily functioning and better longer-term prognosis." That would mean that feeling depressed was outside the spectrum of human experience, that it said nothing about the life of the person – an alien emotion to be excised. I didn’t believe that as an Internist, and I don’t believe it now. I personally find the whole thrust of this way of looking at people strange. It’s like treating someone with a severe headache with analgesics before finding out if they have Migraine, or a brain tumor, or are having a stroke, or a million other things. I agree that there are people with depression that do have a pathological mood state independent of life/mind things. I used to treat them too when I was up on things. Now, when I see them, I send them to friends who are in the business of treating such cases, who see them all the time. But there aren’t so many in that category.

In other posts, I’ve talked about the sorry state of the Clinical Research  Industry and the heavy bias in the Pharmaceutical Industry’s Clinical Trials [the ones Dr. Bernard Carroll calls "experimercials"]. But this study is different with its generous NIMH funding. I’ll even forgo my usual suspicions that the subjects really didn’t really fit the bill diagnostically. But even at that, this study was "fudged" all over the place. The question is why? None of the authors was in the pocket of some drug company whose favorite drug was featured, and yet the whole study reeks of bias. How come? What is the bias of these authors [whom I presume designed this study themselves]?

• Depression, whether it’s a disease or an emotion, is a bad thing  and the point is to make it go away with some form of treatment, usually drugs ["Symptom remission is the desired goal of treatment for depression, given its implications for better daily functioning and better longer-term prognosis"].
• If the treatment doesn’t make it go away, the subject has something called treatment resistance, and should try another treatment ["The number of treatment steps needed to achieve an adequate benefit is typically used to gauge the degree of treatment resistance…"].
• The goal of Psychiatry is to  improve on this treatment scheme ["Studies to identify the best multistep treatment sequences for individual patients and the development of more broadly effective treatments are needed"].

Dr. Rush has served as an advisor, consultant, or speaker for or received research support from Advanced Neuromodulation Systems, Inc.; Best Practice Project Management, Inc.; Bristol-Myers Squibb Company; Cyberonics, Inc.; Eli Lilly & Company; Forest Pharmaceuticals, Inc.; Gerson Lehman Group; GlaxoSmithKline; Healthcare Technology Systems, Inc.; Jazz Pharmaceuticals; Merck & Co., Inc.; the National Institute of Mental Health; Neuronetics; Ono Pharmaceutical; Organon USA Inc.; Personality Disorder Research Corp.; Pfizer Inc.; the Robert Wood Johnson Foundation; the Stanley Medical Research Institute; the Urban Institute; and Wyeth-Ayerst Laboratories Inc. He has equity holdings in Pfizer Inc and receives royalty/patent income from Guilford Publications and Healthcare Technology Systems, Inc.
Dr. Trivedi has served as an advisor, consultant, or speaker for or received research support from Abbott Laboratories, Inc.; Akzo (Organon Pharmaceuticals Inc.); Bayer; Bristol-Myers Squibb Company; Cephalon, Inc.; Corcept Therapeutics, Inc.; Cyberonics, Inc.; Eli Lilly & Company; Forest Pharmaceuticals; GlaxoSmithKline; Janssen Pharmaceutica; Johnson & Johnson PRD; Meade Johnson; the National Institute of Mental Health; the National Alliance for Research in Schizophrenia and Depression; Novartis; Parke-Davis Pharmaceuticals, Inc.; Pfizer Inc; Pharmacia & Upjohn; Predix Pharmaceuticals; Sepracor; Solvay Pharmaceuticals, Inc.; and Wyeth-Ayerst Laboratories.
Dr. Wisniewski has received research support from the National Institute of Mental Health and served as an advisor/consultant for Cyberonics, Inc.
Dr. Nierenberg has served as an advisor, consultant, or speaker for or received research support from Bristol-Myers Squibb Company; Cederroth; Cyberonics, Inc.; Eli Lilly & Company; Forest Pharmaceuticals Inc.; Genaissance; GlaxoSmithKline; Innapharma; Janssen Pharmaceutica; Lichtwer Pharma; the National Institute of Mental Health; the National Alliance for Research in Schizophrenia and Depression; Neuronetics; Organon, Inc.; Pfizer Inc; Sepracor; Shire; Stanley Foundation; and Wyeth-Ayerst Laboratories.
Dr. Stewart has served as an advisor, consultant, or speaker for or received research support from Eli Lilly & Company; GlaxoSmithKline; Organon USA Inc.; Shire; and Somerset.
Dr. Warden has received research support from the National Institute of Mental Health and has equity holdings in Bristol-Myers Squibb Company and Pfizer, Inc.
Dr. Thase has served as an advisor, consultant, or speaker for AstraZeneca; Bristol-Myers Squibb Company; Cephalon, Inc.; Cyberonics, Inc.; Eli Lilly & Company; Forest Laboratories, Inc.; GlaxoSmithKline; Janssen Pharmaceutica; Eli Lilly & Company; Novartis; Organon, Inc.; Pfizer Pharmaceutical; Sanofi Aventis; Sepracor, Inc.; Shire US Inc.; and Wyeth Pharmaceuticals.
Dr. Lavori has served as an advisor, consultant, or speaker for or received research support from Bristol-Myers Squibb Company; Celera Diagnostics Inc; Cyberonics, Inc.; the Department of Veterans Affairs; Forest Pharmaceuticals, Inc.; Glaxo-SmithKline; Leaf Cabrezer Hyman and Bernstein; the National Institutes of Health; and Neuronetics, Inc.
Dr. McGrath has served as an advisor, consultant, or speaker for or received research support from Eli Lilly & Company; GlaxoSmithKline; Lipha Pharmaceuticals; the National Institute of Mental Health; the National Institute on Alcohol Abuse and Alcoholism; New York State Department of Mental Hygiene; Organon, Inc.; Research Foundation for Mental Hygiene (New York State); and Somerset Pharmaceuticals.
Dr. Rosenbaum has served as an advisor, consultant, or speaker for or received research support from Astra-Zeneca; Boehringer-Ingelheim; Bristol-Myers Squibb Company; Cephalon; Compellis; Cyberonics; EPIX; Forest; GlaxoSmithKline; Janssen; Lilly; MedAvante; Neuronetics; Novartis; Orexigen; Organon; Pfizer, Inc; Roche Diagnostics; Sanofi; Schwartz; Somaxon; Somerset; Sepracor; Shire; Supernus; and Wyeth. He has equity holdings in Compellis, Medavante, and Somaxon.
Dr. Sackeim has served as an advisor, consultant, or speaker for or received research support from Cyberonics, Inc.; Eli Lilly & Company; Magstim Ltd.; MECTA Corporation; Neurocrine Biosciences Inc.; Neuronetics Inc.; NeuroPace Inc.; and Pfizer Inc.
Dr. Kupfer has served as an advisor, consultant, or speaker for or received research support from Amersham; the Commonwealth of Pennsylvania; Corcept Corporated; Eli Lilly & Company; F. Hoffmann-La Roche Ltd.; Forest Pharmaceuticals; Lundbeck; the National Institute of Mental Health; Novartis; Pfizer, Inc; Servier Amerique; and Solvay/Wyeth. He has equity holdings in Body Media and Med Avante and receives royalty income from Oxford University Press.
Dr. Fava has served as an advisor, consultant, or speaker for or received research support from Abbott Laboratories; Alkermes; Aspect Medical Systems; Astra-Zeneca; Bayer AG; Biovail Pharmaceuticals, Inc.; BrainCells, Inc.; Bristol-Myers Squibb Company; Cephalon; Compellis; Cypress Pharmaceuticals; Dov Pharmaceuticals; Eli Lilly & Company; EPIX Pharmaceuticals; Fabre-Kramer Pharmaceuticals, Inc.; Forest Pharmaceuticals Inc.; GlaxoSmithKline; Grunenthal GmBH; J & J Pharmaceuticals; Janssen Pharmaceutica; Jazz Pharmaceuticals; Knoll Pharmaceutical Company; Lichtwer Pharma GmbH; Lorex Pharmaceuticals; Lundbeck; MedAvante, Inc.; Novartis; Nutrition 21; Organon Inc.; PamLab, LLC; Pfizer, Inc; PharmaStar; Pharmavite; Roche; Sanofi/Synthelabo; Sepracor; Solvay Pharmaceuticals, Inc.; Somerset Pharmaceuticals; and Wyeth-Ayerst Laboratories. He has equity holdings in Compellis and MedAvante.
Dr. Niederehe, Dr. Lebowitz, and Mr. Luther report no competing interests.